Your search keyword '"Jean-Pierre Levesque"' showing total 94 results

1. Adhesion to E‐selectin primes macrophages for activation through AKT and mTOR

Author

Jakob Begun, Ingrid G. Winkler, Jean-Pierre Levesque, Julie M. Davies, and Kristen J. Radford

Subjects

0301 basic medicine, Immunology, P70-S6 Kinase 1, Mice, 03 medical and health sciences, 0302 clinical medicine, E-selectin, Cell Adhesion, Animals, Immunology and Allergy, Kinase activity, Protein kinase B, Cells, Cultured, PI3K/AKT/mTOR pathway, biology, Chemistry, Cell adhesion molecule, Macrophages, TOR Serine-Threonine Kinases, Cell Biology, Cell biology, 030104 developmental biology, Ribosomal protein s6, biology.protein, Tumor necrosis factor alpha, Endothelium, Vascular, E-Selectin, Proto-Oncogene Proteins c-akt, 030215 immunology

Abstract

The endothelial adhesion protein E-selectin/CD62E is not required for leukocyte homing, unlike closely related family member P-selectin/CD62P. As transmigration through the endothelium is one of the first steps in generating a local immune response, we hypothesized that E-selectin may play additional roles in the early stages of immune activation. We found contact with E-selectin, but not P-selectin or vascular cell adhesion molecule 1 (CD106), induced phosphorylation of protein kinase B (AKT) and nuclear factor-κB in mouse bone marrow-derived macrophages (BMDMs) in vitro. This occurred within 15 min of E-selectin contact and was dependent on phosphatidylinositol-3 kinase activity. Binding to E-selectin activated downstream proteins including mammalian target of rapamycin, p70 ribosomal protein S6 kinase and eukaryotic translation initiation factor 4E-binding protein 1. Functionally, adhesion to E-selectin induced upregulation of CD86 expression and CCL2 secretion. We next asked whether contact with E-selectin impacts further BMDM stimulation. We found enhanced secretion of both interleukin (IL)-10 and CCL2, but not tumor necrosis factor or IL-6 in response to lipopolysaccharide (LPS) stimulation after adhesion to E-selectin. Importantly, adhesion to E-selectin did not polarize BMDMs to one type of response but enhanced both arginase activity and nitric oxide production following IL-4 or LPS stimulation, respectively. In cultured human monocytes, adhesion to E-selectin similarly induced phosphorylation of AKT. Finally, when E-selectin was blocked in vivo in mice, thioglycollate-elicited macrophages showed reduced CD86 expression, validating our in vitro studies. Our results imply functions for E-selectin beyond homing and suggest that E-selectin plays an early role in priming and amplifying innate immune responses.

Published

2021

2. Vincristine-induced peripheral neuropathy is driven by canonical NLRP3 activation and IL-1β release

Author

Alexander Mueller, Alexandra V. Smith, Lena Batoon, Mercedes Monteleone, Kate Schroder, Cheyenne J. Sandrock, Jennifer R. Deuis, Grace Pamo Lawrence, Brandon J. Wainwright, Elissa Tolson, Amanda Mayor, Evelyn Israel Nadar, Irina Vetter, Christelle Adolphe, Jean-Pierre Levesque, Bryan Tay, Hana Starobova, and Allison R. Pettit

Subjects

0301 basic medicine, Chemotherapy, Anakinra, Vincristine, business.industry, medicine.medical_treatment, Immunology, Inflammasome, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Allodynia, Peripheral neuropathy, Tumor progression, Knockout mouse, medicine, Cancer research, Immunology and Allergy, medicine.symptom, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

Vincristine is an important component of many regimens used for pediatric and adult malignancies, but it causes a dose-limiting sensorimotor neuropathy for which there is no effective treatment. This study aimed to delineate the neuro-inflammatory mechanisms contributing to the development of mechanical allodynia and gait disturbances in a murine model of vincristine-induced neuropathy, as well as to identify novel treatment approaches. Here, we show that vincristine-induced peripheral neuropathy is driven by activation of the NLRP3 inflammasome and subsequent release of interleukin-1β from macrophages, with mechanical allodynia and gait disturbances significantly reduced in knockout mice lacking NLRP3 signaling pathway components, or after treatment with the NLRP3 inhibitor MCC950. Moreover, treatment with the IL-1 receptor antagonist anakinra prevented the development of vincristine-induced neuropathy without adversely affecting chemotherapy efficacy or tumor progression in patient-derived medulloblastoma xenograph models. These results detail the neuro-inflammatory mechanisms leading to vincristine-induced peripheral neuropathy and suggest that repurposing anakinra may be an effective co-treatment strategy to prevent vincristine-induced peripheral neuropathy.

Published

2021

3. Bacterial Lipopolysaccharides Suppress Erythroblastic Islands and Erythropoiesis in the Bone Marrow in an Extrinsic and G- CSF-, IL-1-, and TNF-Independent Manner

Author

Ingrid G. Winkler, Rebecca N. Wellburn, Whitney Fleming, Joshua Tay, Bianca Nowlan, Kavita Bisht, Jean-Pierre Levesque, Valerie Barbier, and Crystal McGirr

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, bone marrow, Anemia, Immunology, erythroblastic islands, Inflammation, Cytokine Receptor Gene, Mice, 03 medical and health sciences, 0302 clinical medicine, Sepsis, Granulocyte Colony-Stimulating Factor, medicine, Animals, Immunology and Allergy, Original Research, Innate immune system, Tumor Necrosis Factor-alpha, business.industry, anemia of inflammation, lipopolysaccharides, medicine.disease, hematopoietic stem cells, macrophages, Mice, Inbred C57BL, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Erythropoiesis, Tumor necrosis factor alpha, Bone marrow, medicine.symptom, lcsh:RC581-607, business, erythropoiesis, Interleukin-1, 030215 immunology

Abstract

Anemia of inflammation (AI) is the second most prevalent anemia after iron deficiency anemia and results in persistent low blood erythrocytes and hemoglobin, fatigue, weakness, and early death. Anemia of inflammation is common in people with chronic inflammation, chronic infections, or sepsis. Although several studies have reported the effect of inflammation on stress erythropoiesis and iron homeostasis, the mechanisms by which inflammation suppresses erythropoiesis in the bone marrow (BM), where differentiation and maturation of erythroid cells from hematopoietic stem cells (HSCs) occurs, have not been extensively studied. Here we show that in a mouse model of acute sepsis, bacterial lipopolysaccharides (LPS) suppress medullary erythroblastic islands (EBIs) and erythropoiesis in a TLR-4- and MyD88-dependent manner with concomitant mobilization of HSCs. LPS suppressive effect on erythropoiesis is indirect as erythroid progenitors and erythroblasts do not express TLR-4 whereas EBI macrophages do. Using cytokine receptor gene knock-out mice LPS-induced mobilization of HSCs is G-CSF-dependent whereas LPS-induced suppression of medullary erythropoiesis does not require G- CSF-, IL- 1-, or TNF-mediated signaling. Therefore suppression of medullary erythropoiesis and mobilization of HSCs in response to LPS are mechanistically distinct. Our findings also suggest that EBI macrophages in the BM may sense innate immune stimuli in response to acute inflammation or infections to rapidly convert to a pro-inflammatory function at the expense of their erythropoietic function.

Published

2020

4. Engineering a humanized bone organ model in mice to study bone metastases

Author

Parisa Hesami, Jacqui A. McGovern, Bianca Nowlan, Davide Moi, Boris Michael Holzapfel, Elena M. De-Juan-Pardo, Verena M.C. Quent, Cosmo Orlando Hutmacher, Jean-Pierre Levesque, Elia Piccinini, Cedryck Vaquette, Tatiana Oussenko, Peter W. Zandstra, Felix M. Wunner, Ferdinand Wagner, Roberta Mazzieri, Laure Martine, Dan Jing Wu, Anna Taubenberger, Toby D. Brown, Paul D. Dalton, Dietmar W. Hutmacher, and Soft Tissue Biomech. & Tissue Eng.

Subjects

0301 basic medicine, Male, Bone Morphogenetic Protein 7, Bone Neoplasms, Breast Neoplasms, Biology, Adenocarcinoma, SDG 3 – Goede gezondheid en welzijn, General Biochemistry, Genetics and Molecular Biology, Bone and Bones, Extracellular matrix, 03 medical and health sciences, Mice, Breast cancer, Tissue engineering, Electricity, SDG 3 - Good Health and Well-being, In vivo, medicine, Bone organ, Animals, Humans, Tissue Engineering, Hematopoietic Stem Cell Transplantation, Prostatic Neoplasms, medicine.disease, Extracellular Matrix, Haematopoiesis, Disease Models, Animal, 030104 developmental biology, Primary bone, Immunology, Cancer research, 090301 Biomaterials, Female, Stem cell, 111299 Oncology and Carcinogenesis not elsewhere classified

Abstract

Current in vivo models for investigating human primary bone tumors and cancer metastasis to the bone rely on the injection of human cancer cells into the mouse skeleton. This approach does not mimic species-specific mechanisms occurring in human diseases and may preclude successful clinical translation. We have developed a protocol to engineer humanized bone within immunodeficient hosts, which can be adapted to study the interactions between human cancer cells and a humanized bone microenvironment in vivo. A researcher trained in the principles of tissue engineering will be able to execute the protocol and yield study results within 4-6 months. Additive biomanufactured scaffolds seeded and cultured with human bone-forming cells are implanted ectopically in combination with osteogenic factors into mice to generate a physiological bone 'organ', which is partially humanized. The model comprises human bone cells and secreted extracellular matrix (ECM); however, other components of the engineered tissue, such as the vasculature, are of murine origin. The model can be further humanized through the engraftment of human hematopoietic stem cells (HSCs) that can lead to human hematopoiesis within the murine host. The humanized organ bone model has been well characterized and validated and allows dissection of some of the mechanisms of the bone metastatic processes in prostate and breast cancer.

Published

2017

5. Complement receptor C3aR1 controls neutrophil mobilization following spinal cord injury through physiological antagonism of CXCR2

Author

Gail M. Williams, Frederic A. Meunier, Trisha Jogia, Jean-Pierre Levesque, Linda V. Blomster, Bianca Nowlan, Ellen R. Gillespie, Kate E. Campbell, Marc J. Ruitenberg, Xaria X. Li, Trent M. Woodruff, Esther Jacobson, Geoff W. Osborne, Faith H. Brennan, Kelli P. A. MacDonald, and Stephen M. Taylor

Subjects

Adult, Male, 0301 basic medicine, Neutrophils, Inflammation, Complement receptor, Neuroprotection, Receptors, Interleukin-8B, Mice, Phosphatidylinositol 3-Kinases, Young Adult, 03 medical and health sciences, Chemokine receptor, 0302 clinical medicine, Bone Marrow, Cell Movement, Cell Adhesion, Animals, Humans, PTEN, Tensin, Medicine, Receptor, Anaphylatoxin C5a, Spinal cord injury, Spinal Cord Injuries, PI3K/AKT/mTOR pathway, Mice, Knockout, biology, business.industry, PTEN Phosphohydrolase, General Medicine, medicine.disease, Receptors, Complement, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Neutrophil Infiltration, 030220 oncology & carcinogenesis, Immunology, biology.protein, Wounds and Injuries, Female, medicine.symptom, Transcriptome, business, Research Article

Abstract

Traumatic spinal cord injury (SCI) triggers an acute-phase response that leads to systemic inflammation and rapid mobilization of bone marrow (BM) neutrophils into the blood. These mobilized neutrophils then accumulate in visceral organs and the injured spinal cord where they cause inflammatory tissue damage. The receptor for complement activation product 3a, C3aR1, has been implicated in negatively regulating the BM neutrophil response to tissue injury. However, the mechanism via which C3aR1 controls BM neutrophil mobilization, and also its influence over SCI outcomes, are unknown. Here, we show that the C3a/C3aR1 axis exerts neuroprotection in SCI by acting as a physiological antagonist against neutrophil chemotactic signals. We show that C3aR1 engages phosphatase and tensin homolog (PTEN), a negative regulator of the phosphatidylinositol 3-kinase (PI3K)/AKT pathway, to restrain C-X-C chemokine receptor type 2-driven BM neutrophil mobilization following trauma. These findings are of direct clinical significance as lower circulating neutrophil numbers at presentation were identified as a marker for improved recovery in human SCI. Our work thus identifies C3aR1 and its downstream intermediary, PTEN, as therapeutic targets to broadly inhibit neutrophil mobilization/recruitment following tissue injury and reduce inflammatory pathology.

Published

2019

6. Inhibition of JAK1/2 Tyrosine Kinases Reduces Neurogenic Heterotopic Ossification After Spinal Cord Injury

Author

Kylie A. Alexander, Hsu-Wen Tseng, Whitney Fleming, Beulah Jose, Marjorie Salga, Irina Kulina, Susan M. Millard, Allison R. Pettit, François Genêt, and Jean-Pierre Levesque

Subjects

STAT3 Transcription Factor, 0301 basic medicine, lcsh:Immunologic diseases. Allergy, medicine.drug_class, ruxolitinib, Immunology, JAK- STAT signaling pathway, Monocytes, Tyrosine-kinase inhibitor, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Animals, Janus Kinase Inhibitors, Immunology and Allergy, Phosphorylation, Cells, Cultured, Spinal Cord Injuries, Original Research, Muscle Cells, biology, business.industry, Ossification, Heterotopic, Oncostatin M, Oncostatin M receptor, JAK-STAT signaling pathway, Tyrosine phosphorylation, Janus Kinase 1, X-Ray Microtomography, Janus Kinase 2, Glycoprotein 130, oncostatin M receptor, Immunohistochemistry, 3. Good health, Disease Models, Animal, 030104 developmental biology, chemistry, heterotopic ossification, Cancer research, biology.protein, business, lcsh:RC581-607, Tyrosine kinase, spinal cord injury complications, 030215 immunology

Abstract

Neurogenic heterotopic ossifications (NHO) are very incapacitating complications of traumatic brain and spinal cord injuries (SCI) which manifest as abnormal formation of bone tissue in periarticular muscles. NHO are debilitating as they cause pain, partial or total joint ankylosis and vascular and nerve compression. NHO pathogenesis is unknown and the only effective treatment remains surgical resection, however once resected, NHO can re-occur. To further understand NHO pathogenesis, we developed the first animal model of NHO following SCI in genetically unmodified mice, which mimics most clinical features of NHO in patients. We have previously shown that the combination of (1) a central nervous system lesion (SCI) and (2) muscular damage (via an intramuscular injection of cardiotoxin) is required for NHO development. Furthermore, macrophages within the injured muscle play a critical role in driving NHO pathogenesis. More recently we demonstrated that macrophage-derived oncostatin M (OSM) is a key mediator of both human and mouse NHO. We now report that inflammatory monocytes infiltrate the injured muscles of SCI mice developing NHO at significantly higher levels compared to mice without SCI. Muscle infiltrating monocytes and neutrophils expressed OSM whereas mouse muscle satellite and interstitial cell expressed the OSM receptor (OSMR). In vitro recombinant mouse OSM induced tyrosine phosphorylation of the transcription factor STAT3, a downstream target of OSMR:gp130 signaling in muscle progenitor cells. As STAT3 is tyrosine phosphorylated by JAK1/2 tyrosine kinases downstream of OSMR:gp130, we demonstrated that the JAK1/2 tyrosine kinase inhibitor ruxolitinib blocked OSM driven STAT3 tyrosine phosphorylation in mouse muscle progenitor cells. We further demonstrated in vivo that STAT3 tyrosine phosphorylation was not only significantly higher but persisted for a longer duration in injured muscles of SCI mice developing NHO compared to mice with muscle injury without SCI. Finally, administration of ruxolitinib for 7 days post-surgery significantly reduced STAT3 phosphorylation in injured muscles in vivo as well as NHO volume at all analyzed time-points up to 3 weeks post-surgery. Our results identify the JAK/STAT3 signaling pathway as a potential therapeutic target to reduce NHO development following SCI.

Published

2019

7. Cellular players of hematopoietic stem cell mobilization in the bone marrow niche

Author

Ingrid G. Winkler, Joshua Tay, and Jean-Pierre Levesque

Subjects

0301 basic medicine, medicine.medical_specialty, Stromal cell, Bone Marrow Cells, Biology, 03 medical and health sciences, Internal medicine, Granulocyte Colony-Stimulating Factor, medicine, Animals, Humans, Stem Cell Niche, Progenitor cell, Hematopoietic Stem Cell Mobilization, Hematology, Mesenchymal stem cell, hemic and immune systems, Cell biology, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Immunology, Bone marrow, Stem cell

Abstract

Hematopoietic stem cells (HSC) reside in perivascular regions of the bone marrow (BM) embedded within a complex regulatory unit called the niche. Cellular components of HSC niches include vascular endothelial cells, mesenchymal stromal progenitor cells and a variety of mature hematopoietic cells such as macrophages, neutrophils, and megakaryocytes-further regulated by sympathetic nerves and complement components as described in this review. Three decades ago the discovery that cytokines induce a large number of HSC to mobilize from the BM into the blood where they are easily harvested, revolutionised the field of HSC transplantation-curative for immune-deficiencies and some malignancies. However, despite now routine use of granulocyte-colony stimulating factor (G-CSF) to mobilise HSC for transplant, only in last 15 years has research on the mechanisms behind why and how HSC can be induced to move into the blood began. These studies have revealed the complexity of the niche that retains HSC in the BM. This review describes how BM niches and HSC themselves change during administration of G-CSF-or in the recovery phase of chemotherapy-to facilitate movement of HSC into the blood, and research now leading to development of novel therapeutics to further boost HSC mobilization and transplant success.

Published

2016

8. Concise Review: Humanized Models of Tumor Immunology in the 21st Century: Convergence of Cancer Research and Tissue Engineering

Author

Ferdinand Wagner, Laure Thibaudeau, Jean-Pierre Levesque, Dietmar W. Hutmacher, and Boris Michael Holzapfel

Subjects

Stem cell-microenvironment interactions, Research groups, ved/biology.organism_classification_rank.species, tissue regeneration, Computational biology, Biology, Regenerative Medicine, Regenerative medicine, Translational Research, Biomedical, Tissue engineering, Neoplasms, Animals, Humans, Bone marrow, Bone, Model organism, Adult stem cells, Tissue Engineering, ved/biology, Translational medicine, Cell Biology, 111200 ONCOLOGY AND CARCINOGENESIS, Disease Models, Animal, Murine model, Immunology, 090301 Biomaterials, humanized mice models, Molecular Medicine, Convergence (relationship), Tumor immunology, 111204 Cancer Therapy (excl. Chemotherapy and Radiation Therapy), CD34+, Adult hematopoietic stem cells, Stem Cell Transplantation, Developmental Biology

Abstract

Despite positive testing in animal studies, more than 80% of novel drug candidates fail to proof their efficacy when tested in humans. This is primarily due to the use of preclinical models that are not able to recapitulate the physiological or pathological processes in humans. Hence, one of the key challenges in the field of translational medicine is to “make the model organism mouse more human.” To get answers to questions that would be prognostic of outcomes in human medicine, the mouse's genome can be altered in order to create a more permissive host that allows the engraftment of human cell systems. It has been shown in the past that these strategies can improve our understanding of tumor immunology. However, the translational benefits of these platforms have still to be proven. In the 21st century, several research groups and consortia around the world take up the challenge to improve our understanding of how to humanize the animal's genetic code, its cells and, based on tissue engineering principles, its extracellular microenvironment, its tissues, or entire organs with the ultimate goal to foster the translation of new therapeutic strategies from bench to bedside. This article provides an overview of the state of the art of humanized models of tumor immunology and highlights future developments in the field such as the application of tissue engineering and regenerative medicine strategies to further enhance humanized murine model systems. Stem Cells 2015;33:1696–1704

Published

2015

9. Interaction of c-Myb with p300 is required for the induction of acute myeloid leukemia (AML) by human AML oncogenes

Author

Ingrid G. Winkler, Warren S. Alexander, Jean-Pierre Levesque, Valerie Barbier, Andrew C. Perkins, Keerthana Krishnan, Jianmin Ding, Crystal McGirr, Ann E.O. Trezise, Peter Papathanasiou, Paula L. Hawthorne, Thomas J. Gonda, Pamela Mukhopadhyay, Diwakar R. Pattabiraman, Konstantin Shakhbazov, Sean M. Grimmond, Pattabiraman, Diwakar R, McGirr, Crystal, Shakhbazov, Konstantin, Barbier, Valerie, Krishnan, Keerthana, Mukhopadhyay, Pamela, Hawthorne, Paula, Trezise, Ann, Ding, Jianmin, Grimmond, Sean M, Papathanasiou, Peter, Alexander, Warren S, Perkins, Andrew C, Levesque, Jean Pierre, Winkler, Ingrid G, and Gonda, Thomas J

Subjects

Myeloid, Oncogene Proteins, Fusion, Immunology, Transcription factor complex, P300-CBP Transcription Factors, acute myeloid leukemia, Biology, Biochemistry, Mice, Proto-Oncogene Proteins c-myb, Proto-Oncogene Proteins, hemic and lymphatic diseases, medicine, Animals, Humans, p300-CBP Transcription Factors, MYB, neoplasms, Alleles, Gene Expression Regulation, Leukemic, Gene Expression Profiling, Myeloid leukemia, Oncogenes, Cell Biology, Hematology, medicine.disease, Mice, Mutant Strains, DNA-Binding Proteins, Transplantation, Leukemia, Myeloid, Acute, Leukemia, Cell Transformation, Neoplastic, HEK293 Cells, medicine.anatomical_structure, c-MYB, Core Binding Factor Alpha 2 Subunit, Mutation, Cancer research, Transcription Factors

Abstract

The MYB oncogene is widely expressed in acute leukemias and is important for the continued proliferation of leukemia cells, suggesting that MYB may be a therapeutic target in these diseases. However, realization of this potential requires a significant therapeutic window for MYB inhibition, given its essential role in normal hematopoiesis, and an approach for developing an effective therapeutic. We previously showed that the interactionof c-MybwiththecoactivatorCBP/p300 is essential for its transforming activity. Here, by using cells from Booreana mice which carry a mutant allele of c-Myb, we show that this interaction is essential for in vitro transformation by the myeloid leukemia oncogenes AML1-ETO, AML1-ETO9a, MLL-ENL, and MLL-AF9. We further show that unlike cells from wild-type mice, Booreana cells transduced with AML1-ETO9a or MLL-AF9 retroviruses fail to generate leukemia upon transplantation into irradiated recipients. Finally, we have begun to explore themolecularmechanisms underlying these observations by gene expression profiling. This identified several genes previously implicated in myeloid leukemogenesis and HSC function as being regulated in a c-Myb-p300-dependent manner. These data highlight the importance of the c-Myb-p300 interaction inmyeloid leukemogenesis and suggest disruption of this interaction as a potential therapeutic strategy for acute myeloid leukemia. Refereed/Peer-reviewed

Published

2014

10. Blocking Vascular Niche E-Selectin Dampens AML Stem Cell Regeneration/Survival Potential In Vivo By Inhibiting MAPK/ERK and PI3K/AKT Signalling Pathways

Author

John L. Magnani, Jean-Pierre Levesque, Joshua Tay, Ingrid G. Winkler, Corrine E Fiveash, Johanna D Erbani, and Valerie Barbier

Subjects

MAPK/ERK pathway, Phosphoinositide 3-kinase, biology, Chemistry, Regeneration (biology), Immunology, Cell Biology, Hematology, Biochemistry, Cell biology, Transplantation, hemic and lymphatic diseases, Precursor cell, biology.protein, Stem cell, Selectin, PI3K/AKT/mTOR pathway

Abstract

We have previously shown vascular E (endothelial)-selectin to play a key role in niche-mediated chemo-resistance in Acute Myeloid Leukaemia (AML). Now we report that the cell surface glycosylation of AML blasts -and thus their E-selectin-binding potential- alters during therapy and queried whether these variations influence treatment outcome. Using preclinical mouse models of 11q23-rearranged (MLL-AF9) monomyelocytic AML, we found that although AML blasts in untreated mice display a range of E-selectin-binding potentials, the blasts with highest E-selectin-binding potential dominate in bone marrow (BM) after 24hr cytarabine therapy. Indeed, the highest 10% of AML blasts for E-selectin-binding were >12-fold (p=0.0014) more likely to survive post-chemotherapy. These data raise the question whether E-selectin binding potential itself may prospectively identify AML blasts with heightened regenerative potential. An alternative explanation could be that high-binding AML blasts predominate after chemotherapy simply due to survival advantages mediated by vascular niche E-selectin interaction. To investigate this, BM AML blasts were FACs sorted from donor C57BL/6 mice based on E-selectin-binding potential (highest and lowest 10%) and transplanted into recipient mice (1,500 AML blasts/recipient, 8/gp). No significant differences in duration of disease-free survival was observed. Thus E-selectin-binding potential itself does not prognostically identify the most potent Leukemia Reconstituting Cells (LRC) that initiate relapse. To determine instead whether the AML blasts that bind E-selectin can dominate during stress because of the survival advantage of interacting with E-selectin at the niche, an identical parallel experiment was performed, the only difference being that donor mice had E-selectin blocked (GMI-1271 100mg/kg BiD) for the last 48h prior to BM harvest, FACs sort of AML blasts and recipient mouse transplant. This time we observed a significant (2-fold) extension in disease-free survival in the recipients of high-binding AMLs (from donors treated with GMI-1271) compared to all other groups (p=0.012, median disease-free survival 33 vs. 63 days). Together these data indicate that administration of E-selectin antagonists, even as a single agent, may potentially improve patient outcomes - in cases where heightened E-selectin binding potential is observed. Next we investigated the intracellular AML signaling pathways potentially dampened by E-selectin absence/blockade. Two common pathways used by malignant cells for survival/regeneration are the PI3K/AKT/mTOR/ NF-kB and RAS/MAPK/ERK pathways. We have already shown the absence (in Sele-/- mice), or therapeutic blockade of E-selectin (with GMI-1271) in mice significantly dampens PI3K/AKT/NF-kB signaling in BM AML blasts in vivo. However, AML blasts can utilize alternative pathways such as RAS/MAPK/ERK for survival signaling as well, especially in the 30% of AMLs with NRAS mutations. So we determined whether MAPK/ERK signaling in AML could be similarly altered by E-selectin absence/blockade. Indeed MAPK/ERK phosphorylation was significantly reduced (2-fold) in BM AML blasts from host mice treated 24hr with GMI-1271 and in Sele-/- hosts. Thus contact with vascular E-selectin induces a range of survival/regenerative signaling pathways within BM AML blasts that would be highly advantageous for the blast in times of stress. In summary we show, (1) vascular niche E-selectin blockade by GMI-1271 dampens malignant AML reconstitution/survival potential in vivo when administered as sole agent alone, (2) That E-selectin blockade mediates these effects via dampening a range of intracellular survival/regeneration signalling pathways in the malignant cell, and finally (3) these data suggest E-selectin blockade may synergise with other specific pathway inhibitors to improve treatment outcomes - but only for malignant cells that are appropriately glycosylated to interact with E-selectin. Disclosures Winkler: GlycoMimetics: Patents & Royalties. Levesque:GlycoMimetics: Equity Ownership. Magnani:GlycoMimetics Inc: Employment, Equity Ownership.

Published

2019

11. CD162 Is a Key E-Selectin Receptor Promoting Acute Myeloid Leukemia Chemo-Resistance in the Bone Marrow Niche

Author

Johanna D Erbani, Ingrid G. Winkler, Valerie Barbier, Jean-Pierre Levesque, Joshua Tay, and John L. Magnani

Subjects

biology, business.industry, Cell adhesion molecule, Immunology, Myeloid leukemia, Cell Biology, Hematology, Biochemistry, medicine.anatomical_structure, hemic and lymphatic diseases, E-selectin, biology.protein, Cancer research, Cytarabine, Medicine, L-selectin, Bone marrow, Receptor, business, neoplasms, Selectin, medicine.drug

Abstract

We have recently found that the vascular adhesion molecule E(endothelial)-selectin is a critical bone marrow niche component mediating acute myeloid leukemia (AML) chemo-resistance. Clinical trials involving the use of E-selectin mimetics to improve efficacy of conventional AML therapy are in progress. In this study we investigate the identity of the AML cell surface receptors mediating vascular E-selectin-induced chemo-resistance. E-selectin has two well-characterised receptors, CD162 also known as P-Selectin Glycoprotein Ligand-1 (PSGL-1), and CD44 isoform HCELL (Hematopoietic Cell E-selectin/L-selectin Ligand) with other cell surface glycoproteins (such as ESL-1) and glycolipids also binding E-selectin after Sialyl Lewisx/a glycosylation. To investigate which of these AML cell surface receptors are responsible for mediating vascular E-selectin survival signalling, we first investigated if each co-localized with E-selectin on AML cell surface by confocal imaging. Human CD34+ AML KG1a cells were labelled ± adhesion to fluorescently E-selectin-IgM. Confocal imaging revealed that although both canonical CD44 and CD162 receptors co-localized with E-selectin at the site of cell contact, only CD162 became strongly polarized at E-selectin binding site, while CD44 remained widely distributed across the cell surface. To dissect a functional role for each of these canonical receptors in human AML, CRISPR-Cas9 gene editing was used to selectively delete CD44 and/or CD162 from human AML KG1a cells. We found that although deletion of both CD44 and CD162 receptors reduced KG1a E-selectin-IgM binding potential (3-fold), deletion of either receptor alone did not. Next, we investigated whether deletion of either receptor reversed E-selectin-mediated chemo-resistance in an in vitro chemosensitivity assay. KG1a cells were seeded in wells pre-coated with a range of vascular adhesion molecules commonly expressed in the bone marrow niche, then monitored for cell survival after 48hr treatment ± cytarabine. In this in vitro assay, we found that adhesion to E-selectin significantly increased parental KG1a survival to chemotherapy (p=0.0035). No similar increase in survival was observed following adhesion to P-selectin, or with integrin ligands ICAM-1 and PE-CAM-1. When we repeated the assay using Crispr CD44 deleted KG1a AML we found significant E-selectin-mediated chemo-resistance was still observed (p=0.027) even in the absence of CD44. These results suggest CD44 is not the receptor mediating AML chemo-resistance. In contrast E-selectin-mediated chemo-resistance was abrogated in the CD162 Crispr deleted human KG1a AMLs. Together these data suggest CD162/PSGL-1 expressed on the surface of human AML KG1a appears to be the receptor mediating vascular E-selectin chemo-resistance. This would be a completely novel role described for CD162 which is conventionally known as a homing molecule. To confirm this new role for CD162 in mediating AML chemo-resistance can be replicated in pre-clinical models in vivo, we next generated (11q23-rearranged) AML from CD44-/- and/or CD162-/- gene-deleted mice by retroviral transduction of murine hematopoietic stem cells with MLL-AF9 which then were transplanted into wildtype mice. Cohorts of leukemic mice (n=8/gp) were administered induction therapy (cytarabine/doxorubicin) to monitor impact on disease-free survival. In contrast to AMLs from wildtype, we found absence of CD162 in murine AMLs lead to a pronounced chemo-sensitisation in vivo resulting in a significant (6-fold, p=0.0004) extension in overall disease-free survival duration, compared to either no chemotherapy gene-deleted AML controls, or to treated wildtype AML controls. These in vivo murine data confirm the identification of an exciting new role for CD162 as an important cell surface receptor mediating therapy resistance in AML. In conclusion, we describe a novel form of niche-mediated chemo-resistance and identify CD162 as a key AML cell surface receptor involved in both human and mouse AML therapy resistance. CD162/PSGL-1 expression has not previously been implicated in direct therapy resistance. Together these findings help extend our knowledge on the potential mechanisms by which therapeutic blockade of vascular E-selectin can significantly improves therapy outcomes. Disclosures Levesque: GlycoMimetics: Equity Ownership. Magnani:GlycoMimetics Inc: Employment, Equity Ownership. Winkler:GlycoMimetics: Patents & Royalties.

Published

2019

12. Oncostatin M Is a Novel Niche Factor That Restrains Hematopoietic Stem Cell Mobilization in Response to G-CSF and CXCR4 Antagonist Plerixafor

Author

Kylie A. Alexander, Kavita Bisht, Ingrid G. Winkler, Whitney Fleming, Gerhard Müller Newen, Crystal McGirr, Jean-Pierre Levesque, and Natalie A. Sims

Subjects

CXCR4 antagonist, biology, Plerixafor, Immunology, Oncostatin M, Cell Biology, Hematology, Biochemistry, Granulocyte colony-stimulating factor, Transplantation, medicine, Cancer research, biology.protein, Stromal cell-derived factor 1, Stem cell, Hematopoietic Stem Cell Mobilization, medicine.drug

Abstract

Granulocyte colony-stimulating factor (G-CSF) and the CXCR4 chemokine receptor antagonist Plerixafor are used to mobilize hematopoietic stem and progenitor cells (HSPC). However, in the autologous setting, prior chemotherapy and radiotherapy impair HSPC mobilizing response to G-CSF and Plerixafor thereby precluding autologous HSC transplantation. We now demonstrate in mice that oncostatin M (OSM) production in the bone marrow (BM) is dramatically increased in response to G-CSF and that OSM counteracts the mobilizing effect of G-CSF and Plerixafor indirectly through the BM stroma. Indeed, by immunohistochemistry, a 4-day G-CSF treatment strongly increased OSM protein expression in cell clusters containing F4/80+ macrophages in the endosteal and central region of the mobilized BM. OSM concentration was 7-fold higher in BM fluids of G-CSF mobilized mice compared to control mice as measured by ELISA. To investigate OSM effects on HSPC mobilization, C57BL/6 mice (WT) and mice lacking the OSM receptor gene (OSMR-/-) were treated with 125 μg/kg human G-CSF bidaily for 2-6 days and/or Plerixafor (10 mg/kg) one hour before harvest. Absence of OSMR increased HSPC mobilization with a 4-fold increase in colony forming cells (CFC), phenotypic Lin-Kit+Sca1+ HSPC (LKS+ cells) and LKS+Flt3-CD48-CD150+ HSC into the blood at days 2 and 4 of G-CSF treatment and increased accumulation of HSPC and HSC in the spleen of OSMR-/- mice at day 6 of G-CSF treatment. In a competitive repopulation assay with serial dilutions of mobilized blood, deletion of OSMR gene enhanced ≈4-fold mobilization of functional reconstituting HSC in response to G-CSF as shown by Poisson's distribution analysis. HSPC mobilization in response to Plerixafor was also significantly enhanced with a doubling of CFC, HSPC and HSC into the blood of OSMR-/- mice compared to WT. OSMR gene deletion also significantly enhanced HSPC mobilization (3-fold) in response to G-CSF plus Plerixafor combination, the most effective mobilization regimen currently approved. To further demonstrate that endogenous OSM restrains HSPC mobilization in response to G-CSF, we produced a recombinant mouse OSM-trap, a dimeric protein chimera made of the extracellular domain of mouse OSMR and mouse gp130 fused with a mutant Fc fragment of mouse IgG2a. Co-administration of this OSM-trap together with G-CSF also increased HSPC and HSC mobilization into the blood in response to G-CSF compared to mice treated with G-CSF and control trap construct. This negative effect of endogenous OSM on HSPC mobilization was indirectly mediated by BM stromal cells. qRT-PCR on BM myeloid and stromal cells sorted from steady-state or mobilized mice showed that Osm mRNA is mostly expressed by CD11b+F4/80+CD169+VCAM1+ macrophages and CD11b+F4/80-Ly6G+ neutrophils. In sharp contrast, Osmr mRNA was undetectable in any sorted BM leukocyte population, but abundantly expressed by CD45-Lin-CD31+Sca1+CD105+ endothelial and CD45-Lin-CD31-CD51+PDGFRα+/-Sca-1+/- mesenchymal progenitor cells. OSMR protein was expressed by vascular beds in the BM as detected by IHC. Confirming the indirect effect of OSM, we found that recombinant OSM had no effect on HSPC chemotaxis in response to CXCL12, or HSPC adhesion to immobilized VCAM-1 or selectins in vitro. However, HSPC freshly isolated from the BM of OSMR-/- mice had enhanced chemotaxis in response to CXCL12 compared to HSPC isolated from WT mice. In conclusion, G-CSF increases OSM expression in the BM, and this appears to restrain HSPC mobilization in response to G-CSF via OSMR-expressing endothelial and mesenchymal cells that decreases HSPC responsiveness to CXCL12 gradient. Disclosures Winkler: GlycoMimetics: Patents & Royalties. Levesque:GlycoMimetics: Equity Ownership.

Published

2019

13. Targeting the Hypoxia-Sensing Pathway in Clinical Hematology

Author

Jean-Pierre Levesque and Catherine E. Forristal

Subjects

medicine.medical_specialty, Glycine, Biology, Internal medicine, Basic Helix-Loop-Helix Transcription Factors, medicine, Humans, Hypoxia, Hematology, Plerixafor, Aryl Hydrocarbon Receptor Nuclear Translocator, Hematopoietic stem cell, Anemia, Cell Biology, General Medicine, Hypoxia (medical), Hypoxia-Inducible Factor 1, alpha Subunit, Isoquinolines, Amino Acids, Dicarboxylic, Repressor Proteins, Transplantation, Haematopoiesis, medicine.anatomical_structure, Erythropoietin, Immunology, Cancer research, Bone marrow, medicine.symptom, Apoptosis Regulatory Proteins, Signal Transduction, Stem Cell Transplantation, Perspectives, Developmental Biology, medicine.drug

Abstract

Summary Hypoxia-inducible factors (HIFs) are oxygen-sensitive transcription factors regulated by oxygen-dependent prolyl hydroxylase domain (PHD) enzymes and are key to cell adaptation to low oxygen. The hematopoietic stem cell (HSC) niche in the bone marrow is highly heterogeneous in terms of microvasculature and thus oxygen concentration. The importance of hypoxia and HIFs in the hematopoietic environment is becoming increasingly recognized. Many small compounds that inhibit PHDs have been developed, enabling HIFs to be pharmacologically stabilized in an oxygen-independent manner. The use of PHD inhibitors for therapeutic intervention in hematopoiesis is being increasingly investigated. PHD inhibitors are well established to increase erythropoietin production to correct anemia in hemodialysis patients. Pharmacological stabilization of HIF-1α protein with PHD inhibitors is also emerging as an important regulator of HSC proliferation and self-renewal. Administration of PHD inhibitors increases quiescence and decreases proliferation of HSCs in the bone marrow in vivo, thereby protecting them from high doses of irradiation and accelerating hematological recovery. Recent findings also show that stabilization of HIF-1α increases mobilization of HSCs in response to granulocyte colony-stimulating factor and plerixafor, suggesting that PHD inhibitors could be useful agents to increase mobilization success in patients requiring transplantation. These findings highlight the importance of the hypoxia-sensing pathway and HIFs in clinical hematology

Published

2013

14. Engraftment Outcomes after HPC Co-Culture with Mesenchymal Stromal Cells and Osteoblasts

Author

Valerie Barbier, Katarina Kollar, Matthew M. Cook, Ingrid G. Winkler, Michael R. Doran, Kerry Atkinson, Gary Brooke, and Jean-Pierre Levesque

Subjects

haematopoietic reconstitution, Stromal cell, Cell, lcsh:Medicine, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, Progenitor cell, 030304 developmental biology, 0303 health sciences, haematopoietic stem cells, mesenchymal stromal cells, osteoblasts, ex vivo expansion, business.industry, Mesenchymal stem cell, lcsh:R, Osteoblast, General Medicine, 090300 BIOMEDICAL ENGINEERING, Transplantation, Haematopoiesis, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, Cancer research, Stem cell, business

Abstract

Haematopoietic stem cell (HSC) transplantation is an established cell-based therapy for a number of haematological diseases. To enhance this therapy, there is considerable interest in expanding HSCs in artificial niches prior to transplantation. This study compared murine HSC expansion supported through co-culture on monolayers of either undifferentiated mesenchymal stromal cells (MSCs) or osteoblasts. Sorted Lineage(-) Sca-1(+) c-kit(+) (LSK) haematopoietic stem/progenitor cells (HPC) demonstrated proliferative capacity on both stromal monolayers with the greatest expansion of LSK shown in cultures supported by osteoblast monolayers. After transplantation, both types of bulk-expanded cultures were capable of engrafting and repopulating lethally irradiated primary and secondary murine recipients. LSKs co-cultured on MSCs showed comparable, but not superior, reconstitution ability to that of freshly isolated LSKs. Surprisingly, however, osteoblast co-cultured LSKs showed significantly poorer haematopoietic reconstitution compared to LSKs co-cultured on MSCs, likely due to a delay in short-term reconstitution. We demonstrated that stromal monolayers can be used to maintain, but not expand, functional HSCs without a need for additional haematopoietic growth factors. We also demonstrated that despite apparently superior in vitro performance, co-injection of bulk cultures of osteoblasts and LSKs in vivo was detrimental to recipient survival and should be avoided in translation to clinical practice.

Published

2013

15. Role of bone marrow macrophages in controlling homeostasis and repair in bone and bone marrow niches

Author

Simranpreet Kaur, Allison R. Pettit, Lena Batoon, Liza J. Raggatt, Jean-Pierre Levesque, and David A. Hume

Subjects

0301 basic medicine, Niche, Biology, Bone and Bones, 03 medical and health sciences, 0302 clinical medicine, Bone Marrow, bone and bone marrow, medicine, Animals, Homeostasis, Humans, Stem Cell Niche, Ecological niche, Wound Healing, Resident tissue macrophage, Macrophages, Cell Biology, haematopoiesis, Stem cell niche, macrophages, Cell biology, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, Bone marrow, stem cell niches, Developmental Biology

Abstract

Macrophages, named for their phagocytic ability, participate in homeostasis, tissue regeneration and inflammatory responses. Bone and adjacent marrow contain multiple functionally unique resident tissue macrophage subsets which maintain and regulate anatomically distinct niche environments within these interconnected tissues. Three subsets of bone-bone marrow resident tissue macrophages have been characterised; erythroblastic island macrophages, haematopoietic stem cell niche macrophages and osteal macrophages. The role of these macrophages in controlling homeostasis and repair in bone and bone marrow niches is reviewed in detail.

Published

2016

16. Nichotherapy for stem cells: There goes the neighborhood

Author

John E.J. Rasko, Ingrid G. Winkler, and Jean-Pierre Levesque

Subjects

Ecological niche, Plerixafor, Niche, Hematopoietic Stem Cell Transplantation, Bone Marrow Cells, Biology, Hematopoietic Stem Cells, medicine.disease, Hematopoietic Stem Cell Mobilization, General Biochemistry, Genetics and Molecular Biology, Granulocyte colony-stimulating factor, Leukemia, Neoplasms, Immunology, medicine, Animals, Humans, Stem Cell Niche, Progenitor cell, Stem cell, Neuroscience, medicine.drug

Abstract

Stem cells and their malignant counterparts require the support of a specific microenvironment or "niche". While various anti-cancer therapies have been broadly successful, there are growing opportunities to target the environment in which these cells reside to further improve therapeutic efficacy and outcome. This is particularly true when the aim is to target normal or malignant stem cells. The field aiming to target or use the niches that harbor, protect, and support stem cells could be designated as "nichotherapy". In this essay, we provide a few examples of nichotherapies. Some have been employed for decades, such as hematopoietic stem cell mobilization, whereas others are emerging, such as chemosensitization of leukemia stem cells by targeting their niche.

Published

2012

17. Mobilisation strategies for normal and malignant cells

Author

Alison M. Rice, David Gottlieb, Linda J. Bendall, Vicki Antonenas, John E.J. Rasko, Ingrid G. Winkler, Susan K. Nilsson, Julian Cooney, Devendra K Hiwase, Ashanka Beligaswatte, Stephen R Larsen, Jean-Pierre Levesque, L. Bik To, Antony C. Cambareri, Anthony K. Mills, Ian D. Lewis, and Kirsten Herbert

Subjects

Transplantation Conditioning, business.industry, Mesenchymal stem cell, Hematopoietic Stem Cell Transplantation, Bone Marrow Stem Cell, Mesenchymal Stem Cells, Stem cell factor, Hematopoietic Stem Cells, medicine.disease, Hematopoietic Stem Cell Mobilization, Pathology and Forensic Medicine, Granulocyte colony-stimulating factor, Transplantation, Graft-versus-host disease, Granulocyte macrophage colony-stimulating factor, Models, Animal, Immunology, medicine, Cancer research, Animals, Humans, Stem cell, business, medicine.drug

Abstract

This review evaluates the latest information on the mobilisation of haemopoietic stem cells for transplantation, with the focus on what is the current best practice and how new understanding of the bone marrow stem cell niche provides new insights into optimising mobilisation regimens. The review then looks at the mobilisation of mesenchymal stromal cells, immune cells as well as malignant cells and what clinical implications there are.

Published

2011

18. How we mobilize haemopoietic stem cells

Author

L. B. To, Kirsten Herbert, John E.J. Rasko, Anthony K. Mills, David Gottlieb, Julian Cooney, Jeff Szer, and Jean-Pierre Levesque

Subjects

medicine.medical_specialty, Mobilization, business.industry, medicine.medical_treatment, Plerixafor, Hematopoietic stem cell transplantation, Transplantation, Immunology, Internal Medicine, Medicine, Autologous transplantation, Progenitor cell, Stem cell, business, Intensive care medicine, Hematopoietic Stem Cell Mobilization, medicine.drug

Abstract

Mobilization and collection of haemopoietic stem and progenitor cells (HSPC) is the cornerstone of autologous and allogeneic stem cell transplantation for a wide variety of haematological and some non-haematological malignancies. Centres providing this service face the challenge of optimizing the likelihood of successful collection of transplantable doses of cells, while maximizing the efficiency of the apheresis unit and minimizing the risk of toxicity as well as mobilization failure. Recent developments in the understanding of the molecular mechanisms of mobilization have led to the emergence of novel strategies for HSPC mobilization, which may assist in meeting these imperatives. The task for clinicians is how to incorporate the use of these strategies into practice, in the light of emerging evidence for efficacy and safety of these agents. Herein, the literature is reviewed, and a proposed algorithm for HSPC mobilization is presented.

Published

2011

19. Hierarchy of immature hematopoietic cells related to blood flow and niche

Author

Ingrid G. Winkler and Jean-Pierre Levesque

Subjects

Hematopoietic System, Mesenchymal stem cell, Niche, Hematopoietic stem cell, hemic and immune systems, Cell Growth Processes, Hematology, Biology, Hematopoietic Stem Cells, Cell biology, Blood cell, Haematopoiesis, medicine.anatomical_structure, Immunology, medicine, Animals, Humans, Bone marrow, Stem Cell Niche, Stem cell, Progenitor cell, Signal Transduction

Abstract

Purpose of Review: Steady-state hematopoiesis in adult bone marrow requires the maintenance of a small pool of hematopoietic stem cells (HSCs) by self-renewing symmetric division. HSCs can be divided into potent rarely dividing HSCs which function as long-term reserve and more proliferative HSCs which contribute to maintaining the blood and immune cell pool. Extrinsic instructions provided by unique microenvironments (niches) regulate the fate of individual HSCs and progenitors. This review discusses the latest findings in respect to the organization and function of these niches. Recent Findings: It has recently emerged that mesenchymal stem cells, various osteoblastic progenitors and sinusoidal endothelial cells all critically regulate HSCs within niches. Each of these niche cells expresses different arrays of signaling proteins which differentially regulate HSCs and progenitors. HSCs have been reported in two types of niches. However, as osteoblastic/mesenchymal niches and perivascular niches overlap anatomically, this makes the dichotomy between osteoblastic niches for quiescent HSCs and endothelial niches for more proliferative HSCs a too simplistic model. Indeed local blood perfusion in a niche alone can functionally separate HSC populations. SUMMARY: The fate of each individual HSC is likely to be the result of the unique balance between signals elicited by proteins expressed by mesenchymal/osteoblastic progenitors, sinusoidal endothelial cells and physicochemical cues such as local blood perfusion and hypoxia in each individual niche. More sophisticated three-dimensional fluorescence microscopy techniques on whole mount bone fragments should provide new insights in the spatial organization of niches relative to bone and microcirculation in the bone marrow.

Published

2011

20. Vascular E-Selectin Acts As a Gatekeeper Inducing Commitment and Loss of Self-Renewal in HSC Transmigrating through the Marrow Vasculature

Author

Paula Marlton, Joshua Tay, Anthony K. Mills, Johanna Erbani, Jessica Lowe, Andrew C. Perkins, Corrine E Fiveash, Ingrid G. Winkler, Jean-Pierre Levesque, John L. Magnani, and Valerie Barbier

Subjects

biology, Endothelium, P-selectin, Cell adhesion molecule, business.industry, Immunology, Cell Biology, Hematology, Biochemistry, Cell biology, Transplantation, medicine.anatomical_structure, E-selectin, medicine, biology.protein, Stromal cell-derived factor 1, Bone marrow, business, Selectin

Abstract

Hematopoietic stem cells (HSC) reside in specific peri-vascular niches in the bone marrow (BM). We have shown interactions with the inflammatory vascular adhesion molecule E-(endothelial)-selectin awakens HSC (Nat Med 2012). We now report that BM vascular cell-surface E-selectin expression is strongly upregulated during HSC mobilization regimens raising the question of a role for endothelial E-selectin in HSC transplant outcome. G-CSF was administered to cohorts of E gene-deleted or wildtype C57BL/6 mice together with E-selectin antagonist Uproleselan (Upro, GMI-1271). We found absence (Sele-/- mice) or therapeutic blockade (Upro) of E-selectin alone in steady-state hosts did not alter levels of circulating peripheral blood (PB) HSC. In contrast absence or therapeutic blockade of E-selectin strongly synergized with mobilizing regimens such as G-CSF or cyclophosphamide+G-CSF by boosting long-term engraftment and reconstitution potential of mobilized blood. The effect was pronounced boosting reconstitution potential over G-CSF-alone-mobilized blood 24-fold ( Two hypotheses may explain how therapeutic E-selectin-blockade promotes potency of mobilized HSC;Dampening of inflammatory activation at the BM niche induced by G-CSF that drive HSC exhaustion,Directly preventing adhesion-mediated HSC commitment during trans-endothelial transmigration from BM into blood. To investigate inflammatory mediator profiles in the BM, cohorts of mice were administered saline control or G-CSF ± Upro (125ug/kg G-CSF, 40mg/kg Upro BiD for 3 days) then femoral BM fluids flushed for cytokine profiling (LegendPlex). As anticipated, G-CSF administration significantly increased concentration of classic pro-inflammatory cytokines (TNF-α, IL-1β, IL-23, IFN-β) in BM associated with HSC activation and loss of quiescence in the BM. No similar boost in inflammatory mediators was observed in BM from mobilized mice co-administered Upro. Similarly pronounced metabolic changes could be observed in BM HSC following in vivo G-CSF administration (such as a significant doubling in HSC Mitochondrial Membrane potential [MOMP] suggesting increased energy demands with HSC activation) was similarly reversed in vivo by Upro co-administration. Together these results suggest blockade of E-selectin on activated vasculature significantly dampens BM HSC activation following G-CSF administration - potentially shielding HSC self-renewal potential. Next we investigated whether the transient interactions with endothelial E-selectin during trans-endothelial transmigration from BM into blood also directly affects HSC potency. BM HSPC harvested from G-CSF plus Upro-treated mice were loaded in transwells pre-coated with recombinant adhesion molecules (P-selectin, E-selectin and CD14-Fc as control) and HSC induced to transmigrate through coated pores towards CXCL12 gradient. After 3hr cell numbers were enumerated and exactly 100 transmigrated HSC from each well transplanted/recipient in a LT-CR transplant assay. Analysis of % CD45.2+ donor HSC reconstitution confirmed a pronounced 10-fold drop in reconstitution potential of HSC transmigrated through E-selectin compared to P-selectin or control coated transwells (p=0.0027) confirming that transient adhesive interactions with E-selectin, such as would occur on activated vasculature during HSC transmigration from BM into the blood, strongly impact subsequent HSC reconstitution upon transplantation. In summary, transient interactions between intravasating HSC with E-selectin on BM vasculature inadvertently compromises reconstitution potential of up to 96% of conventionally harvested HSC, indicating an unexpected disadvantage with current HSC harvesting procedures. These studies also point the way forward to a simple remedy, administration of E-selectin antagonist (Upro) together with G-CSF during HSC mobilization, to improve HSC transplant outcomes. Disclosures Winkler: GlycoMimetics: Patents & Royalties. Magnani:GlycoMimetics: Employment, Equity Ownership, Membership on an entity's Board of Directors or advisory committees. Marlton:Celgene: Membership on an entity's Board of Directors or advisory committees; Novartis: Honoraria, Membership on an entity's Board of Directors or advisory committees; AbbVie: Honoraria, Membership on an entity's Board of Directors or advisory committees; GlycoMimetics: Research Funding; Pfizer: Membership on an entity's Board of Directors or advisory committees; Astellas: Honoraria, Membership on an entity's Board of Directors or advisory committees; Janssen: Honoraria, Membership on an entity's Board of Directors or advisory committees; Roche: Honoraria, Membership on an entity's Board of Directors or advisory committees. Perkins:Novartis Oncology: Honoraria. Levesque:GlycoMimetics: Equity Ownership, Patents & Royalties.

Published

2018

21. Prostaglandin I2 in the Endosteal Bone Marrow Niche As a Novel Regulator of Hematopoietic Stem Cells

Author

Ingrid G. Winkler, Falak Helwani, Jean-Pierre Levesque, Bianca Nowlan, Joshua Tay, Gareth Price, and Valerie Barbier

Subjects

Immunology, Regulator, Prostaglandin, Cell Biology, Hematology, Biology, Colony-stimulating factor, Biochemistry, Cell biology, Granulocyte colony-stimulating factor, Transplantation, chemistry.chemical_compound, Haematopoiesis, medicine.anatomical_structure, chemistry, medicine, Bone marrow, Stem cell

Abstract

Haematopoietic stem cells (HSCs) are regulated by their immediate microenvironment or niche. The most potent functional HSCs are enriched at the endosteum near the bone, which comprises ~10% of total bone marrow (BM). To identify novel niche factors that regulate HSCs, we performed a gene expression microarray seeking genes that were >2-fold overexpressed in the endosteal BM relative to the central BM. In this screen, we uncovered known essential HSC niche factors overexpressed in the endosteal BM such as Scf, Cxcl12, and Angpt1, which validated our approach. Among the genes overexpressed in the endosteal BM, prostaglandin I2 (PGI2) synthase (Ptgis) was one of the highest enriched genes in the endosteum (>10-fold by qRT-PCR, p In initial experiments where we cultured fluorescence activated cell sorted (FACS) BM lineage- Kit+ Sca-1- (LKS+) haematopoietic stem and progenitor cells (HSPCs) for 7 days in serum free conditions, we found iloprost treatment potently reduced proliferation and differentiation compared to vehicle controls, assessed by flow cytometry phenotyping (p We next sought to determine whether iloprost affects HSC function in vivo. In steady state, low dose 0.1mg/kg iloprost administration to mice for 15 days did not alter BM HSPC phenotypes by flow cytometry nor HSC reconstitution potential in competitive transplants compared to vehicle controls suggesting PGI2 does not alter HSC function in homeostasis. To further test the effect of PGI2 following stress, mice were sub-lethally (6.5 Gy) irradiated or administered pro-inflammatory granulocyte colony stimulating factor (G-CSF) for 3 days. We found low dose iloprost administration partially rescued BM HSC reconstitution potential 21 days following irradiation (p To understand the extrinsic mechanisms through which PGI2 regulates HSC in the BM following stress, we performed a HSC homing assay using naïve donors transplanted into 2-day G-CSF administered recipients. Analysis of HSPC homing to the BM at 4 hours post-transplantation revealed ~4-fold greater proportion of LKS+ HSPC homing to the BM of iloprost co-administered recipients compared to vehicle controls (p In summary, we have identified PGI2 as a novel HSC niche factor abundant in the endosteal BM. PGI2 analogues like Iloprost are well-tolerated and used clinically to treat vascular diseases such as pulmonary arterial hypertension and Raynaud's phenomenon. Our research suggests that PGI2 analogues can be rapidly repurposed in the clinic to improve HSC transplant outcomes and protect against BM failure following acute stressors such as accidental irradiation or inflammation. Disclosures Levesque: GlycoMimetics: Equity Ownership, Patents & Royalties.

Published

2018

22. Bone marrow macrophages maintain hematopoietic stem cell (HSC) niches and their depletion mobilizes HSCs

Author

Kylie A. Alexander, Nico van Rooijen, Bianca Nowlan, Jean-Pierre Levesque, Natalie A. Sims, Ingrid G. Winkler, Ingrid J. Poulton, Falak Helwani, Liza J. Raggatt, Valerie Barbier, Allison R. Pettit, Molecular cell biology and Immunology, and CCA - Immuno-pathogenesis

Subjects

Hematopoietic stem cell niche, Immunology, Population, Bone Marrow Cells, Cell Separation, Biology, Biochemistry, Mice, Cell Movement, Granulocyte Colony-Stimulating Factor, medicine, Animals, Cell Lineage, Stem Cell Niche, education, Mice, Knockout, Endosteum, education.field_of_study, Reverse Transcriptase Polymerase Chain Reaction, Macrophages, Hematopoietic stem cell, Cell Differentiation, Osteoblast, Cell Biology, Hematology, Flow Cytometry, Hematopoietic Stem Cells, Immunohistochemistry, Cell biology, Mice, Inbred C57BL, Haematopoiesis, medicine.anatomical_structure, Bone marrow, Stem cell

Abstract

In the bone marrow, hematopoietic stem cells (HSCs) reside in specific niches near osteoblast-lineage cells at the endosteum. To investigate the regulation of these endosteal niches, we studied the mobilization of HSCs into the bloodstream in response to granulocyte colony-stimulating factor (G-CSF). We report that G-CSF mobilization rapidly depletes endosteal osteoblasts, leading to suppressed endosteal bone formation and decreased expression of factors required for HSC retention and self-renewal. Importantly, G-CSF administration also depleted a population of trophic endosteal macrophages (osteomacs) that support osteoblast function. Osteomac loss, osteoblast suppression, and HSC mobilization occurred concomitantly, suggesting that osteomac loss could disrupt endosteal niches. Indeed, in vivo depletion of macrophages, in either macrophage Fas-induced apoptosis (Mafia) transgenic mice or by administration of clodronate-loaded liposomes to wild-type mice, recapitulated the: (1) loss of endosteal osteoblasts and (2) marked reduction of HSC-trophic cytokines at the endosteum, with (3) HSC mobilization into the blood, as observed during G-CSF administration. Together, these results establish that bone marrow macrophages are pivotal to maintain the endosteal HSC niche and that the loss of such macrophages leads to the egress of HSCs into the blood.

Published

2010

23. The endosteal ‘osteoblastic’ niche and its role in hematopoietic stem cell homing and mobilization

Author

Jean-Pierre Levesque, Ingrid G. Winkler, and Falak Helwani

Subjects

Cancer Research, Cell type, Sympathetic Nervous System, Niche, Genes, myc, Bone Marrow Cells, Biology, Cell Movement, Osteogenesis, medicine, Animals, Humans, Stem Cell Niche, Progenitor cell, Hematopoietic Stem Cell Mobilization, Osteoblasts, Hematopoietic stem cell, Osteoblast, Hematology, Hematopoietic Stem Cells, Cell biology, medicine.anatomical_structure, Oncology, Immunology, Calcium, Osteopontin, Bone marrow, Homing (hematopoietic)

Abstract

The concept of hematopoietic stem cell (HSC) niche was formulated in 1978, but HSC niches remained unidentified for the following two decades largely owing to technical limitations. Sophisticated live microscopy techniques and genetic manipulations have identified the endosteal region of the bone marrow (BM) as a preferential site of residence for the most potent HSC - able to reconstitute in serial transplants - with osteoblasts and their progenitors as critical cellular elements of these endosteal niches. This article reviews the path to the discovery of these endosteal niches (often called 'osteoblastic' niches) for HSC, what cell types contribute to these niches with their known physical and biochemical features. In the past decade, a first wave of research uncovered many mechanisms responsible for HSC homing to, and mobilization from, the whole BM tissue. However, the recent discovery of endosteal HSC niches has initiated a second wave of research focusing on the mechanisms by which most primitive HSC lodge into and migrate out of their endosteal niches. The second part of this article reviews the current knowledge of the mechanisms of HSC lodgment into, retention in and mobilization from osteoblastic niches.

Published

2010

24. Hematopoietic Progenitor Cell Mobilization Results in Hypoxia with Increased Hypoxia-Inducible Transcription Factor-1α and Vascular Endothelial Growth Factor A in Bone Marrow

Author

Ingrid G. Winkler, Jean Hendy, Susan K. Nilsson, Valerie Barbier, Brenda Williams, Jean-Pierre Levesque, Falak Helwani, and Bianca Nowlan

Subjects

Male, Vascular Endothelial Growth Factor A, Bone Marrow Cells, Mice, Inbred Strains, Vascular permeability, Biology, Capillary Permeability, Mice, Oxygen Consumption, Bone Marrow, Cell Movement, Tumor Cells, Cultured, medicine, Animals, Progenitor cell, Transcription factor, Mice, Inbred BALB C, Hematopoietic stem cell, Cell Biology, Hematopoietic Stem Cells, Hypoxia-Inducible Factor 1, alpha Subunit, Cell Hypoxia, Cell biology, Mice, Inbred C57BL, Haematopoiesis, Vascular endothelial growth factor A, medicine.anatomical_structure, Gene Expression Regulation, Nitroimidazoles, Immunology, Molecular Medicine, Bone marrow, Stem cell, Granulocytes, Developmental Biology

Abstract

Despite the fact that many hypoxia-inducible genes are important in hematopoiesis, the spatial distribution of oxygen in the bone marrow (BM) has not previously been explored in vivo. Using the hypoxia bioprobe pimonidazole, we showed by confocal laser scanning microscopy that the endosteum at the bone-BM interface is hypoxic, with constitutive expression of hypoxia-inducible transcription factor-1α (HIF-1α) protein in steady-state mice. Interestingly, at the peak of hematopoietic stem and progenitor cell (HSPC) mobilization induced by either granulocyte colony-stimulating factor or cyclophosphamide, hypoxic areas expand through the central BM. Furthermore, we found that HSPC mobilization leads to increased levels of HIF-1α protein and increased expression of vascular endothelial growth factor A (VEGF-A) mRNA throughout the BM, with an accumulation of VEGF-A protein in BM endothelial sinuses. VEGF-A is a cytokine known to induce stem cell mobilization, vasodilatation, and vascular permeability in vivo. We therefore propose that the expansion in myeloid progenitors that occurs during mobilization depletes the BM hematopoietic microenvironment of O2, leading to local hypoxia, stabilization of HIF-1α transcription factor in BM cells, increased transcription of VEGF-A, and accumulation of VEGF-A protein on BM sinuses that increases vascular permeability.Disclosure of potential conflicts of interest is found at the end of this article.

Published

2007

25. Granulocyte Colony-Stimulating Factor and an RAR?? Specific Agonist, VTP195183, Synergize to Enhance the Mobilization of Hematopoietic Progenitor Cells

Author

Ingrid G. Winkler, Kirsten Herbert, Carl R. Walkley, H. Miles Prince, Gemma Haines Olsen, Jean Hendy, Roshantha A.S. Chandraratna, Louise E. Purton, Jean-Pierre Levesque, and Yang-Dar Yuan

Subjects

Agonist, Time Factors, Neutrophils, Receptors, Retinoic Acid, medicine.drug_class, Guanosine Monophosphate, Tretinoin, Biology, Granulocyte, Neutrophil Activation, Mice, Bone Marrow, Cell Movement, Granulocyte Colony-Stimulating Factor, medicine, Animals, Humans, Progenitor cell, Cells, Cultured, Transplantation, Mobilization, Retinoic Acid Receptor alpha, Hematopoietic Stem Cells, Granulocyte colony-stimulating factor, Haematopoiesis, medicine.anatomical_structure, Immunology, Cancer research, Bone marrow, Stem cell, Peptide Hydrolases

Abstract

Failure to mobilize adequate numbers of hematopoietic stem and progenitor cells (HSPC) is an important clinical problem. Since bone marrow (BM) neutrophils play a central role in HSPC mobilization, we hypothesized that granulocyte colony-stimulating factor (G-CSF)-mediated mobilization would be enhanced by further expanding the size of the BM granulocyte pool.We tested the potential of the retinoic acid receptor alpha (RARalpha) specific agonist VTP195183, and the pan-RAR agonist all-trans retinoic acid (ATRA), to enhance G-CSF-mediated mobilization of HSPC, in two mouse strains.Pretreatment of mice with VTP195183 significantly increased the number of leukocytes, colony-forming cells, and early engrafting hematopoietic stem cells (HSC) mobilized in the blood in response to G-CSF. In contrast, ATRA had only a marginal effect on G-CSF-induced mobilization. HSPC mobilization synergy between VTP195183 and G-CSF occurred only when mice were preconditioned with VTP195183 prior to G-CSF. This preconditioning was shown to increase the numbers of granulocyte/macrophage progenitors in the BM. Treatment with VTP195183 and G-CSF was accompanied by enhanced levels of active neutrophil proteases in the BM extracellular fluid compared to G-CSF treatment alone.VTP195183 treatment increases the numbers of immature granulocyte progenitors in BM and subsequently synergizes to enhance G-CSF-mediated mobilization of HSPC. These data demonstrate a novel approach to improve G-CSF-induced mobilization by accelerating granulocyte maturation in the BM. These findings are currently being tested in a clinical trial of VTP195183 plus G-CSF for mobilization of HSPC in human patients.

Published

2007

26. Filling the void: allogeneic myeloid cells for transplantation

Author

Lars K. Nielsen, Jessica L. Schwaber, Marion E. G. Brunck, and Jean-Pierre Levesque

Subjects

0301 basic medicine, medicine.medical_treatment, Primary Cell Culture, Cord Blood Stem Cell Transplantation, Hematopoietic stem cell transplantation, Biology, 03 medical and health sciences, medicine, Humans, Transplantation, Homologous, Myeloid Cells, Progenitor cell, Clinical Trials as Topic, Graft Survival, Hematopoietic Stem Cell Transplantation, Hematology, Cellular Reprogramming, Hematopoietic Stem Cells, Transplantation, Haematopoiesis, surgical procedures, operative, 030104 developmental biology, medicine.anatomical_structure, Treatment Outcome, Batch Cell Culture Techniques, Immunology, Bone marrow, Stem cell, Homing (hematopoietic)

Abstract

PURPOSE OF REVIEW The success of allogeneic haematopoietic stem and progenitor cell (HSPC) transplantations remains inconsistent. Umbilical cord blood (UCB) is a promising source of HSPCs for transplantation, but low cell yield hampers its widespread use. Multiple strategies are being developed to manipulate UCB to either increase HSPC content or enhance bone marrow homing upon transfusion. RECENT FINDINGS Several ex-vivo manipulation protocols have increased engraftment success in recent phase I/II clinical trials. Additionally, by exploiting knowledge of the transcriptome, mature cells were dedifferentiated into induced haematopoietic stem cells capable of self-renewal and reconstitution of haematopoiesis in vivo. SUMMARY UCB is a more readily available source of allogeneic transplant material compared with bone marrow and mobilized peripheral blood. However, the number of HSPCs in a graft is correlated to the rate and success of engraftment and UCB grafts typically contain 10 times less cells compared with bone marrow or mobilized peripheral blood grafts that contain around 1 × 10⁸ CD34⁺ cells. Recently, research efforts have focused on increasing UCB engrafting cells in addition to the methods to accelerate engraftment or to provide transient protection and support until engraftment succeeds.

Published

2015

27. G-CSF potently inhibits osteoblast activity and CXCL12 mRNA expression in the bone marrow

Author

Jean-Pierre Levesque, Daniel C. Link, F. Patrick Ross, Paul J. Simmons, Ingrid G. Winkler, Matthew J. Christopher, Fulu Liu, Jean Chappel, Brenton Short, and Craig L. Semerad

Subjects

medicine.medical_specialty, Stromal cell, Immunology, Down-Regulation, Granulocyte, Biochemistry, Mice, Bone Marrow, Cell Movement, Internal medicine, Granulocyte Colony-Stimulating Factor, medicine, Animals, Humans, Stromal cell-derived factor 1, RNA, Messenger, Receptor, Cells, Cultured, Osteoblasts, biology, Cell Membrane, Osteoblast, Cell Biology, Hematology, Hematopoietic Stem Cells, biological factors, Chemokine CXCL12, Hematopoiesis, Cell biology, Haematopoiesis, medicine.anatomical_structure, Endocrinology, biology.protein, Osteocalcin, Bone marrow, Chemokines, CXC

Abstract

Accumulating evidence indicates that interaction of stromal cell-derived factor 1 (SDF-1/CXCL12 [CXC motif, ligand 12]) with its cognate receptor, CXCR4 (CXC motif, receptor 4), generates signals that regulate hematopoietic progenitor cell (HPC) trafficking in the bone marrow. During granulocyte colony-stimulating factor (G-CSF)–induced HPC mobilization, CXCL12 protein expression in the bone marrow decreases. Herein, we show that in a series of transgenic mice carrying targeted mutations of their G-CSF receptor and displaying markedly different G-CSF–induced HPC mobilization responses, the decrease in bone marrow CXCL12 protein expression closely correlates with the degree of HPC mobilization. G-CSF treatment induced a decrease in bone marrow CXCL12 mRNA that closely mirrored the fall in CXCL12 protein. Cell sorting experiments showed that osteoblasts and to a lesser degree endothelial cells are the major sources of CXCL12 production in the bone marrow. Interestingly, osteoblast activity, as measured by histomorphometry and osteocalcin expression, is strongly down-regulated during G-CSF treatment. However, the G-CSF receptor is not expressed on osteoblasts; accordingly, G-CSF had no direct effect on osteoblast function. Collectively, these data suggest a model in which G-CSF, through an indirect mechanism, potently inhibits osteoblast activity resulting in decreased CXCL12 expression in the bone marrow. The consequent attenuation of CXCR4 signaling ultimately leads to HPC mobilization.

Published

2005

28. Epitope recognition of antibodies that define the sialomucin, endolyn (CD164), a negative regulator of haematopoiesis

Author

James Yi Hsin Chan, R A Dwek, Pauline M. Rudd, Regis Doyonnas, B. Jorgensen-Tye, Suzanne M. Watt, Louise Royle, D.J. Harvey, P.J. Simmons, and Jean-Pierre Levesque

Subjects

Peanut agglutinin, Glycosylation, Sialomucins, medicine.drug_class, Immunology, Tn antigen, CD146 Antigen, Biology, Monoclonal antibody, Biochemistry, Endolyn, Epitope, Antigen-Antibody Reactions, Mice, chemistry.chemical_compound, Agglutinin, Antigens, CD, Lectins, Genetics, medicine, Animals, Humans, Immunology and Allergy, Neural Cell Adhesion Molecules, Chromatography, High Pressure Liquid, Immunodominant Epitopes, Mucins, Antibodies, Monoclonal, SIGLEC, Exons, General Medicine, Molecular biology, Recombinant Proteins, Hematopoiesis, Sialic acid, chemistry, Agglutinins, biology.protein, Epitope Mapping, Transcription Factors

Abstract

Endolyn (CD164) is a sialomucin that functions as an adhesion molecule and a negative regulator of CD34+ CD38- human haematopoietic precursor cell proliferation. The 105A5 and 103B2/9E10 CD164 monoclonal antibodies (mAbs), which act as surrogate ligands, recognize distinct glycosylation-dependent classes I and II epitopes located on domain I of the native and recombinant CD164 proteins. Here, we document five new CD164 mAbs, the 96 series, that rely on conformational integrity, but not glycosylation, of exons 2- and 3-encoded CD164 domains, thereby resembling the class III mAbs, N6B6 and 67D2. Although all the 96 series class III mAbs labelled both the 105A5+ and 103B2/9E10+ cells, cross-competition and immunoblotting studies allow them to be categorized into two distinct class III subgroups, i.e. the N6B6-like subgroup that only recognizes 80-100 kDa proteins and the 67D2-like subgroup that also recognizes a higher molecular weight (>220 kDa) form. To more closely define the reactivity patterns of mAbs to the classes I and II epitopes, the global glycosylation patterns of the soluble human (h) CD164 proteins were determined using lectin binding, high-performance liquid chromatography (HPLC) and mass spectrometry. hCD164 recombinant proteins bound to the lectins, Galanthus nivalis agglutinin, Datura stramonium agglutinin, Sambucus nigra agglutinin, Maackia amurensis agglutinin and peanut agglutinin, indicating the presence of high mannose and complex N-glycans, in addition to core 1 O-glycans (the Tn antigen) and alpha2-3 and alpha2-6 sialic acid moieties. Our HPLC and mass spectrometry results revealed both high mannose and complex N-glycosylation with various numbers of branches increasing the complexity of the glycosylation pattern. Most O-glycans were small, core 1 or 2 based. High levels of sialylation in alpha2-3 and alpha2-6 linkages, without sialyl-Lewis X, indicate that the majority of these hCD164 recombinant proteins are unable to bind to selectins in our assay system, but may interact with Siglec molecules.

Published

2005

29. Characterization of hematopoietic progenitor mobilization in protease-deficient mice

Author

Fulu Liu, Robert M. Senior, Christine T.N. Pham, Daniel C. Link, Paul J. Simmons, Jean-Pierre Levesque, and Tomoko Betsuyaku

Subjects

Proteases, Cathepsin G, Stromal cell, Neutrophils, Immunology, Vascular Cell Adhesion Molecule-1, Mice, Transgenic, Matrix Metalloproteinase Inhibitors, Granulocyte, Biology, Biochemistry, Cathepsin C, Colony-Forming Units Assay, Mice, chemistry.chemical_compound, Bone Marrow, Endopeptidases, Granulocyte Colony-Stimulating Factor, medicine, Animals, Humans, Protease Inhibitors, Mice, Knockout, Interleukin-8, Serine Endopeptidases, Cell Biology, Hematology, Hematopoietic Stem Cells, Cathepsins, Molecular biology, Chemokine CXCL12, Hematopoietic Stem Cell Mobilization, Recombinant Proteins, Mice, Inbred C57BL, Haematopoiesis, medicine.anatomical_structure, Matrix Metalloproteinase 9, chemistry, Neutrophil elastase, biology.protein, Receptors, Chemokine, Bone marrow, Chemokines, CXC

Abstract

Recent evidence suggests that protease release by neutrophils in the bone marrow may contribute to hematopoietic progenitor cell (HPC) mobilization. Matrix metalloproteinase-9 (MMP-9), neutrophil elastase (NE), and cathepsin G (CG) accumulate in the bone marrow during granulocyte colony-stimulating factor (G-CSF) treatment, where they are thought to degrade key substrates including vascular cell adhesion molecule-1 (VCAM-1) and CXCL12. To test this hypothesis, HPC mobilization was characterized in transgenic mice deficient in one or more hematopoietic proteases. Surprisingly, HPC mobilization by G-CSF was normal in MMP-9–deficient mice, NE × CG-deficient mice, or mice lacking dipeptidyl peptidase I, an enzyme required for the functional activation of many hematopoietic serine proteases. Moreover, combined inhibition of neutrophil serine proteases and metalloproteinases had no significant effect on HPC mobilization. VCAM-1 expression on bone marrow stromal cells decreased during G-CSF treatment of wild-type mice but not NE × CG-deficient mice, indicating that VCAM-1 cleavage is not required for efficient HPC mobilization. G-CSF induced a significant decrease in CXCL12α protein expression in the bone marrow of Ne × CG-deficient mice, indicating that these proteases are not required to down-regulate CXCL12 expression. Collectively, these data suggest a complex model in which both protease-dependent and -independent pathways may contribute to HPC mobilization.

Published

2004

30. Radio-resistant recipient bone marrow (BM) macrophages (MACS) are necessary for hematopoietic stem cell (HSC) engraftment post transplantation

Author

Ingrid G. Winkler, Kelli P. A. MacDonald, Allison R. Pettit, Andrew C. Perkins, Rebecca Jacobsen, David A. Hume, Simranpreet Kaur, Liza J. Raggatt, Jean-Pierre Levesque, Susan M. Millard, and Lena Batoon

Subjects

0301 basic medicine, Cancer Research, medicine.diagnostic_test, biology, Hematopoietic stem cell, Spleen, Cell Biology, Hematology, Transplantation Chimera, Molecular biology, Flow cytometry, Transplantation, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Integrin alpha M, Immunology, Genetics, medicine, biology.protein, Bone marrow, Molecular Biology

Abstract

For decades it has been assumed that lethal irradiation in bone marrow transplantation experiments ablates the entire host hematopoietic system but preserves the host non-hematopoietic bone marrow stroma. This postulate is at the basis of transplantation chimera experiments in mice to test involvement of hematopoietic cells versus non-hematopoietic stroma. As BM-Macs support HSC niche homeostasis, we examined whether host-derived BM-Macs persist lethal irradiation and play a role in HSC engraftment. Recipient MacGreen mice (expressing GFP in myeloid cells under the control of Csf1r promoter) were lethally irradiated (11.5Gy) and transplanted with sorted syngeneic B6.SJL CD45.1+ Lin-Kit+Sca1+ sorted cells. Flow cytometry analyses of BM 2-30 weeks (wk) post-transplant confirmed more than 99% donor chimerism of monocytes and granulocytes validating ablation of recipient HSC. In contrast, GFP+CD11b+F4/80+CD169+VCAM-1+ERHR3+Ly6Gneg recipient BM-Macs were detected throughout the time-course. A 5.9 fold expansion of these recipient BM-Macs occurred between wk 2 and 5 ( from 45,000 to 270,000 cells/femur) post-transplant which coincided with increased number of phenotypic donor HSC (GFP-Lin-Kit+Sca1+CD48-CD150+). Host BM-Mac proliferation was cell autonomous in the absence of host HSC and granulocytes. Recipient Macs in spleen displayed different frequency and longevity kinetics that correlated with transient post-Tx splenic extramedullary haematopoiesis. In situ, GFP+F480+ recipient BM-Macs were enriched in perivascular microenvironments within both central BM and endosteal regions. These GFP+ host-derived macrophages persisted long-term forming 8.4% of BM macrophages 7months post-transplant. To evaluate the importance of these host-derived radiation-resistant macrophages, we selectively depleted recipient BM-Macs using CD169-DTR mice transplanted with syngeneic ubiquitous GFP+ HSC. Depletion of recipient CD169+ Macs abated engraftment of donor phenotypic HSC by 70% at 5 wk post-transplant and reduced BM reconstitution potential in competitive secondary transplants. In conclusion BM contains a myeloablation-resistant self-repopulating Mac subset that is necessary for efficient and/or sustained HSC BM engraftment following transplantation. Therefore interpretation of transplantation chimera experiments must take into account the persistence of this subset of host macrophages that support donor HSC engraftment.

Published

2016

31. Tissue engineered humanized bone supports human hematopoiesis in vivo

Author

Boris Michael Holzapfel, Daniela Loessner, Judith A. Clements, Jean-Pierre Levesque, Ingrid G. Winkler, John D. Hooper, Bianca Nowlan, Allison R. Pettit, Dietmar W. Hutmacher, Laure Thibaudeau, Pamela J. Russell, Christina Theodoropoulos, and Valerie Barbier

Subjects

Biophysics, Bioengineering, Biology, Biomaterials, Mice, Tissue engineering, Osteogenesis, Bone organ, Animals, Humans, Progenitor cell, Stem Cell Niche, Cells, Cultured, Bone Development, Osteoblasts, Bioartificial Organs, Tissue Engineering, Tissue Scaffolds, Mesenchymal stem cell, Cell Differentiation, Mesenchymal Stem Cells, Equipment Design, Cell biology, Hematopoiesis, Transplantation, Equipment Failure Analysis, Mice, Inbred C57BL, Haematopoiesis, Mechanics of Materials, Immunology, Bone Substitutes, Ceramics and Composites, Female, Stem cell, Homing (hematopoietic)

Abstract

Advances in tissue-engineering have resulted in a versatile tool-box to specifically design a tailored microenvironment for hematopoietic stem cells (HSCs) in order to study diseases that develop within this setting. However, most current in vivo models fail to recapitulate the biological processes seen in humans. Here we describe a highly reproducible method to engineer humanized bone constructs that are able to recapitulate the morphological features and biological functions of the HSC niches. Ectopic implantation of biodegradable composite scaffolds cultured for 4 weeks with human mesenchymal progenitor cells and loaded with rhBMP-7 resulted in the development of a chimeric bone organ including a large number of human mesenchymal cells which were shown to be metabolically active and capable of establishing a humanized microenvironment supportive of the homing and maintenance of human HSCs. A syngeneic mouse-to-mouse transplantation assay was used to prove the functionality of the tissue-engineered ossicles. We predict that the ability to tissue engineer a morphologically intact and functional large-volume bone organ with a humanized bone marrow compartment will help to further elucidate physiological or pathological interactions between human HSCs and their native niches.

Published

2015

32. Hypoxia inducible factor (HIF)-2α accelerates disease progression in mouse models of leukemia and lymphoma but is not a poor prognosis factor in human AML

Author

Ingrid G. Winkler, Richard J D'Andrea, Anna L. Brown, Bianca Nowlan, Andrew C.W. Zannettino, Robert Powell, Jean-Pierre Levesque, Grant A Engler, Sally Martin, Catherine E. Forristal, I D Lewis, Sonya M. Diakiw, Falak Helwani, Diwakar R. Pattabiraman, Valerie Barbier, Forristal, CE, Brown, Alex, Helwani, FM, Winkler, IG, Nowlan, B, Barbier, V, Powell, RJ, Engler, GA, Diakiw, SM, Zannettino, AC, Martin, S, Pattabiraman, D, D'Andrea, Richard, Lewis, ID, and Levesque, JP

Subjects

Adult, Male, Cancer Research, Myeloid, Adolescent, Lymphoma, Preleukemia, Blotting, Western, Mice, Transgenic, Biology, Real-Time Polymerase Chain Reaction, Cohort Studies, Immunoenzyme Techniques, Mice, Young Adult, hemic and lymphatic diseases, medicine, Basic Helix-Loop-Helix Transcription Factors, Animals, Humans, RNA, Messenger, Cells, Cultured, Aged, Neoplasm Staging, Aged, 80 and over, Reverse Transcriptase Polymerase Chain Reaction, Myeloid leukemia, Hematology, Middle Aged, medicine.disease, Hematopoietic Stem Cells, Prognosis, Cell Hypoxia, Transplantation, Survival Rate, Leukemia, Haematopoiesis, Disease Models, Animal, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Oncology, Immunology, Disease Progression, Female, Stem cell, Follow-Up Studies

Abstract

Hypoxia-inducible factor (HIF)-1α accumulation promotes hematopoietic stem cells' quiescence and is necessary to maintain their self-renewal. However, the role of HIF-2α in hematopoietic cells is less clear. We investigated the role of HIF-2α in leukemia and lymphoma cells. HIF-2α expression was high in subsets of human and mouse leukemia and lymphoma cells, whereas it was low in normal bone marrow leukocytes. To investigate the role of HIF-2α, we transduced human HIF-2α cDNA in mouse syngeneic models of myeloid preleukemia and a transgenic model of B lymphoma. Ectopic expression of HIF-2α accelerated leukemia cell proliferation in vitro. Mice transplanted with cells transduced with HIF-2α died significantly faster of leukemia or B lymphoma than control mice transplanted with empty vector-transduced cells. Conversely, HIF-2α knockdown in human myeloid leukemia HL60 cells decreased proliferation in vitro and significantly prolonged animal survival following transplantation. In human acute myeloid leukemia (AML), HIF-2α mRNA was significantly elevated in several subsets such as the t(15;17), inv(16), complex karyotype and favorable cytogenetic groups. However, patients with high HIF-2α expression had a trend to higher disease-free survival in univariate analysis. The different effects of HIF-2α overexpression in mouse models of leukemia and human AML illustrates the complexity of this mutliclonal disease. Refereed/Peer-reviewed

Published

2015

33. Mobilization by either cyclophosphamide or granulocyte colony-stimulating factor transforms the bone marrow into a highly proteolytic environment

Author

Ingrid G. Winkler, Paul J. Simmons, Brenda Williams, Jean Hendy, Yasushi Takamatsu, and Jean-Pierre Levesque

Subjects

Cancer Research, Time Factors, Vascular Cell Adhesion Molecule-1, Bone Marrow Cells, Biology, Cathepsin G, Granulocyte, Mice, chemistry.chemical_compound, Endopeptidases, Granulocyte Colony-Stimulating Factor, Genetics, medicine, Animals, Humans, Progenitor cell, Cyclophosphamide, Molecular Biology, Mice, Inbred BALB C, Myelosuppressive Chemotherapy, Cell Biology, Hematology, Flow Cytometry, Hematopoietic Stem Cells, Hematopoietic Stem Cell Mobilization, Granulocyte colony-stimulating factor, Kinetics, Haematopoiesis, medicine.anatomical_structure, chemistry, Neutrophil elastase, Immunology, biology.protein, Female, Bone marrow

Abstract

Objective. Hematopoietic stem and progenitor cells normally reside in the bone marrow but can be mobilized into the peripheral blood following treatment with granulocyte colony-stimulating factor (G-CSF) or myelosuppressive chemotherapy. Although the number of transplants performed with mobilized blood currently exceeds those performed with bone marrow, little is known of the molecular mechanisms responsible for this phenomenon. We sought to determine whether mobilization induced by G-CSF or chemotherapy was triggered by common or distinct mechanisms. Methods. Balb/c mice were mobilized with either G-CSF alone, cyclophosphamide alone, or the combination of both agents. Spleens, peripheral blood, bone marrow extracellular fluids, and cells were taken at different time points and analyzed for the expression of VCAM-1, the number of peripheral blood progenitor cells, concentration of neutrophil proteases, and number of granulocytes. Results. Administration of either G-CSF or the myelosuppressive agent cyclophosphamide results in a sharp reduction of VCAM-1/CD106 expression in the bone marrow that coincides with the accumulation of granulocytic precursors and release of active neutrophil proteases neutrophil elastase and cathepsin G that directly cleave VCAM-1/CD106 in vitro. These events follow precisely the kinetics of hematopoietic progenitor cell mobilization into the peripheral blood. Conclusion. We have identified a commonality of events during mobilization induced by either G-CSF or chemotherapy, which include the accumulation in the bone marrow of active neutrophil proteases that directly cleave VCAM-1 and lead to the sharp reduction of VCAM-1 expression in this tissue.

Published

2002

34. HIF-1α is required for hematopoietic stem cell mobilization and 4-prolyl hydroxylase inhibitors enhance mobilization by stabilizing HIF-1α

Author

Carl R. Walkley, Gail Walkinshaw, Ingrid G. Winkler, Valerie Barbier, Jean-Pierre Levesque, Bianca Nowlan, Rebecca Jacobsen, and Catherine E. Forristal

Subjects

Male, Cancer Research, Benzylamines, Receptors, CXCR4, Anti-HIV Agents, medicine.medical_treatment, Blotting, Western, Mice, Transgenic, Hematopoietic stem cell transplantation, Biology, Cyclams, Real-Time Polymerase Chain Reaction, CXCR4, Transplantation, Autologous, Prolyl Hydroxylases, Mice, Cell Movement, Heterocyclic Compounds, Granulocyte Colony-Stimulating Factor, medicine, Autologous transplantation, Animals, Humans, RNA, Messenger, Hematopoietic Stem Cell Mobilization, Cells, Cultured, Cell Proliferation, Reverse Transcriptase Polymerase Chain Reaction, Plerixafor, Hematopoietic Stem Cell Transplantation, Prolyl-Hydroxylase Inhibitors, Hematology, Flow Cytometry, Hematopoietic Stem Cells, Hypoxia-Inducible Factor 1, alpha Subunit, Granulocyte colony-stimulating factor, Mice, Inbred C57BL, Haematopoiesis, Oncology, Immunology, Cancer research, Original Article, Stem cell, medicine.drug

Abstract

Many patients with hematological neoplasms fail to mobilize sufficient numbers of hematopoietic stem cells (HSCs) in response to granulocyte colony-stimulating factor (G-CSF) precluding subsequent autologous HSC transplantation. Plerixafor, a specific antagonist of the chemokine receptor CXCR4, can rescue some but not all patients who failed to mobilize with G-CSF alone. These refractory poor mobilizers cannot currently benefit from autologous transplantation. To discover alternative targetable pathways to enhance HSC mobilization, we studied the role of hypoxia-inducible factor-1α (HIF-1α) and the effect of HIF-1α pharmacological stabilization on HSC mobilization in mice. We demonstrate in mice with HSC-specific conditional deletion of the Hif1a gene that the oxygen-labile transcription factor HIF-1α is essential for HSC mobilization in response to G-CSF and Plerixafor. Conversely, pharmacological stabilization of HIF-1α with the 4-prolyl hydroxylase inhibitor FG-4497 synergizes with G-CSF and Plerixafor increasing mobilization of reconstituting HSCs 20-fold compared with G-CSF plus Plerixafor, currently the most potent mobilizing combination used in the clinic.

Published

2014

35. Osteoclast-Mediated Bone Resorption Is Stimulated During Short-Term Administration of Granulocyte Colony-Stimulating Factor But Is Not Responsible for Hematopoietic Progenitor Cell Mobilization

Author

Robert J. Moore, Luen B. To, Paul J. Simmons, Howard A. Morris, Jean-Pierre Levesque, and Yasushi Takamatsu

Subjects

medicine.medical_specialty, Deoxypyridinoline, biology, business.industry, Osteoporosis, Immunology, Cell Biology, Hematology, medicine.disease, Biochemistry, Bone resorption, Resorption, chemistry.chemical_compound, medicine.anatomical_structure, Endocrinology, chemistry, Osteoclast, Internal medicine, medicine, Osteocalcin, biology.protein, Bone marrow, business, Hematopoietic Stem Cell Mobilization

Abstract

The cellular and molecular mechanisms responsible for hematopoietic progenitor cell (HPC) mobilization from bone marrow (BM) into peripheral blood after administration of cytokines such as granulocyte colony-stimulating factor (G-CSF) are still unknown. In this study we show that high concentrations of soluble calcium induce the detachment of BM CD34+ HPC adherent on fibronectin, a major component of BM extracellular matrix. Because G-CSF has been shown to induce osteoporosis in patients with congenital neutropenia and in G-CSF–overexpressing transgenic mice, we hypothesized that short-term G-CSF administration may be sufficient to induce bone resorption, resulting in the release of soluble calcium in the endosteum leading in turn to the inhibition of attachment to fibronectin and the egress of HPC from the BM. We show herein that in humans, serum osteocalcin concentration, a specific marker of bone formation, is strongly reduced after 3 days of G-CSF administration. Furthermore, in patients mobilized with G-CSF either alone or in association with stem cell factor or interleukin-3, the reduction of serum osteocalcin is significantly correlated with the number of HPC mobilized in peripheral blood. Urine levels of deoxypyridinoline (DPyr), a specific marker of bone resorption, gradually elevated during the time course of G-CSF administration until day 7 after cessation of G-CSF, showing a simultaneous stimulation of bone degradation during G-CSF–induced HPC mobilization. In an in vivo murine model, we found that the number of osteoclasts was dramatically increased paralleling the elevation of DPyr after G-CSF administration. When pamidronate, an inhibitor of osteoclast-mediated bone resorption, was administered together with G-CSF in mice, the G-CSF–induced increase of DPyr levels was completely abolished whereas the numbers of colony-forming cells mobilized in peripheral blood were not decreased, but unexpectedly increased relative to the numbers elicited by G-CSF alone. Collectively, our data therefore show that short-term administration of G-CSF induces bone degradation by a simultaneous inhibition of bone formation and an enhanced osteoclast-mediated bone resorption. This increased bone resorption is inhibited by pamidronate without reducing G-CSF–induced HPC mobilization, suggesting that the activation of bone resorption after G-CSF administration is not the direct cause of HPC mobilization as initially hypothesized, but a parallel event.© 1998 by The American Society of Hematology.

Published

1998

36. Stem Cell Factor as a Single Agent Induces Selective Proliferation of the Philadelphia Chromosome Positive Fraction of Chronic Myeloid Leukemia CD34+ Cells

Author

Louise A. McDiarmid, Jean-Pierre Levesque, David N. Haylock, Paul J. Simmons, Leanne M. Samels, Sarah Moore, L. Bik To, and Timothy P. Hughes

Subjects

Immunology, CD34, Myeloid leukemia, Stem cell factor, Cell Biology, Hematology, CD38, Biology, medicine.disease, Biochemistry, Cell culture, hemic and lymphatic diseases, Cancer research, medicine, Progenitor cell, Stem cell, neoplasms, Chronic myelogenous leukemia

Abstract

The interaction between p145(o-KIT) and p210(bcr-abl), transduced cell lines, and the selective outgrowth of normal progenitors during long-term culture of chronic myeloid leukemia (CML) cells on stroma deficient in stem-cell factor (SCF) suggests that the response of CML cells to SCF may be abnormal. We examined the proliferative effect of SCF(100 ng/mL), provided as the sole stimulus, on individual CD34(+) cells from five normal donors and five chronic-phase CML patients. Forty-eight percent of isolated single CML CD34(+) cells proliferated after 6 days of culture to a mean of 18 cells, whereas only 8% of normal CD34(+) cells proliferated (mean number of cells generated was 4). SCF, as a single agent, supported the survival and expansion of colony-forming unit-granulocyte-macrophage (CFU-GM) from CML CD34(+)CD38(+) cells and the more primitive CML CD34(+)CD38(-) cells. These CFU-GM colonies were all bcr-abl positive, showing the specificity of SCF stimulation for the leukemic cell population. Coculture of CML and normal CD34(+) cells showed exclusive growth of Phi cells, suggesting that growth in SCF alone is not dependent on secretion of cytokines by CML cells. SCF augmentation of beta(1)-integrin-mediated adhesion of CML CD34(+) cells to fibronectin was not increased when compared with the effect on normal CD34(+) cells, suggesting that the proliferative and adhesive responses resulting from SCF stimulation are uncoupled. The increased proliferation may contribute to the accumulation of leukemic progenitors, which is a feature of CML, (C) 1998 by The American Society of Hematology.

Published

1998

37. A rapid streptavidin-capture ELISA specific for the detection of antibodies to feline foamy virus

Author

Martin Löchelt, Jochen Bodem, Rolf M. Flügel, Ingrid G. Winkler, Jean-Pierre Levesque, and Robert L. Flower

Subjects

Streptavidin, Immunoblotting, Immunology, Gene Expression, Gene Products, gag, Enzyme-Linked Immunosorbent Assay, Antibodies, Viral, Polymerase Chain Reaction, Veterinarians, law.invention, chemistry.chemical_compound, Biotin, Antigen, Antibody Specificity, Neutralization Tests, law, Prevalence, Animals, Humans, Immunology and Allergy, Cloning, Molecular, Recombination, Genetic, biology, Group-specific antigen, Virology, Molecular biology, Fusion protein, Recombinant Proteins, Antisense Elements (Genetics), chemistry, DNA, Viral, Cats, biology.protein, Recombinant DNA, Spumavirus, Antibody, Clone (B-cell biology), Retroviridae Infections

Abstract

We report a simple procedure for the rapid development of an ELISA with the potential for wide application to any defined protein antigen. The procedure involves the expression of protein encoded by a PCR product, using a commercially available T-vector that adds a biotin tag, and a single step purification by affinity for streptavidin for direct use in ELISA. In our experiments, a recombinant protein from the nucleocapsid domain of the feline foamy virus gag gene was expressed as a fusion protein with a biotin tag and then applied directly to streptavidin-coated ELISA wells. An extract from a clone with the insert in antisense orientation was used as a control. Non-specific reactions with antigen extracts from both sense and antisense clones were observed in 6 of the 376 (1.6%) sera tested. Antibody to feline foamy virus, which forms a stable persistent infection in cats, was detected in 107 of 201 (53%) Australian cats, but none of 175 sera from veterinarians. There was a 100% correlation between FeFV antibody detected by ELISA, immunoblot, serum neutralisation and virus isolation, confirming that this test is sensitive and specific.

Published

1997

38. CD44-Mediated Adhesiveness of Human Hematopoietic Progenitors to Hyaluronan Is Modulated by Cytokines

Author

Stéphane Legras, Florence Smadja-Joffe, Jean-Pierre Levesque, Denis Clay, Kohji Morimoto, Claude Jasmin, Rachida Sihem Charrad, and Caroline Le Bousse

Subjects

medicine.medical_treatment, Immunology, CD34, Antigens, CD34, Bone Marrow Cells, Stem cell factor, Biology, Biochemistry, Colony-Forming Units Assay, Antigens, CD, Cell Adhesion, medicine, Humans, Hyaluronic Acid, Progenitor cell, ADP-ribosyl Cyclase, N-Glycosyl Hydrolases, Interleukin 3, Stem Cell Factor, Membrane Glycoproteins, Cell adhesion molecule, CD44, Histocompatibility Antigens Class II, Antibodies, Monoclonal, Granulocyte-Macrophage Colony-Stimulating Factor, Cell Biology, Hematology, Hematopoietic Stem Cells, ADP-ribosyl Cyclase 1, Antigens, Differentiation, Molecular biology, Clone Cells, Hyaluronan Receptors, medicine.anatomical_structure, Cytokine, biology.protein, Cytokines, Tetradecanoylphorbol Acetate, Interleukin-3, Bone marrow

Abstract

Adhesive interactions between CD34+ hematopoietic progenitor cells (HPC) and bone marrow stroma are crucial for normal hematopoiesis, yet their molecular bases are still poorly elucidated. We have investigated whether cell surface proteoglycan CD44 can mediate adhesion of human CD34+ HPC to immobilized hyaluronan (HA), an abundant glycosaminoglycan of the bone marrow extracellular matrix. Our data show that, although CD34+ cells strongly express CD44, only 13.3% ± 1.1% spontaneously adheres to HA. Short-term methylcellulose assay showed that HA-adherent CD34+ cells comprised granulo-monocytic and erythroid committed progenitors (19.6% ± 2.5% and 7.3% ± 1.0% of the input, respectively). More primitive progenitors, such as pre–colony-forming units, also adhered to HA. Moreover, we found that CD44-mediated adhesion of CD34+ cells to HA could be enhanced by phorbol 12-myristate 13-acetate (PMA), the function-activating anti-CD44 monoclonal antibody H90, and cytokines such as granulocyte-monocyte colony-stimulating factor, interleukin-3 (IL-3), and stem cell factor. Enhancement through PMA required several hours, was protein-synthesis–dependent, and was associated with an increase of CD44 cell surface expression, whereas stimulation of adhesion by H90 monoclonal antibody and cytokines was very rapid and without alteration of CD44 expression. H90-induced activation occurred at 4°C and lasted for at least 2 hours, whereas activation by cytokines required incubation at 37°C and was transient. These data, which show for the first time that CD34+ HPC can directly adhere to HA via CD44, point out that this adhesive interaction to HA is a process that may also be physiologically regulated by cytokines.

Published

1997

39. Mobilization with granulocyte colony-stimulating factor blocks medullar erythropoiesis by depleting F4/80(+)VCAM1(+)CD169(+)ER-HR3(+)Ly6G(+) erythroid island macrophages in the mouse

Author

Nico van Rooijen, Jean-Pierre Levesque, Ingrid G. Winkler, Catherine E. Forristal, Allison R. Pettit, Liza J. Raggatt, Bianca Nowlan, Rebecca Jacobsen, Valerie Barbier, Simranpreet Kaur, Molecular cell biology and Immunology, and CCA - Immuno-pathogenesis

Subjects

Cancer Research, Innate immune system, Macrophages, Hematopoietic stem cell, Vascular Cell Adhesion Molecule-1, Cell Biology, Hematology, Biology, Granulocyte, Cell biology, Granulocyte colony-stimulating factor, Haematopoiesis, Mice, medicine.anatomical_structure, Immunology, Granulocyte Colony-Stimulating Factor, Genetics, medicine, Macrophage, Erythropoiesis, Animals, Bone marrow, Molecular Biology

Abstract

Similarly to other tissues, the bone marrow contains subsets of resident tissue macrophages, which are essential to maintain bone formation, functional hematopoietic stem cell (HSC) niches, and erythropoiesis. Pharmacologic doses of granulocyte colony-stimulating factor (G-CSF) mobilize HSC in part by interfering with the HSC niche-supportive function of BM resident macrophages. Because bone marrow macrophages are key to both maintenance of HSC within their niche and erythropoiesis, we investigated the effect of mobilizing doses of G-CSF on erythropoiesis in mice. We now report that G-CSF blocks medullar erythropoiesis by depleting the erythroid island macrophages we identified as co-expressing F4/80, vascular cell adhesion molecule-1, CD169, Ly-6G, and the ER-HR3 erythroid island macrophage antigen. Both broad macrophage depletion, achieved by injecting clodronate-loaded liposomes, and selective depletion of CD169 + macrophages, also concomitantly depleted F4/80 + VCAM-1 + CD169 + ER-HR3 + Ly-6G + erythroid island macrophages and blocked erythropoiesis. This more precise phenotypic definition of erythroid island macrophages will enable studies on their biology and function in normal settings and on diseases associated with anemia. Finally, this study further illustrates that macrophages are a potent relay of innate immunity and inflammation on bone, hematopoietic, and erythropoietic maintenance. Agents that affect these macrophages, such as G-CSF, are likely to affect these three processes concomitantly.

Published

2013

40. It takes nerves to recover from chemotherapy

Author

Jean-Pierre Levesque and Ingrid G. Winkler

Subjects

Sympathetic Nervous System, Regeneration (biology), Antineoplastic Agents, General Medicine, Biology, Hematopoietic Stem Cells, General Biochemistry, Genetics and Molecular Biology, Article, Endothelial stem cell, Haematopoiesis, medicine.anatomical_structure, Bone Marrow, Immunology, Cancer research, medicine, Cytotoxic T cell, Animals, Regeneration, Female, Bone marrow, Stem cell, Progenitor cell, Adult stem cell

Abstract

Anti-cancer chemotherapy drugs challenge hematopoietic tissues to regenerate, but commonly produce long-term sequelae. Deficits in hematopoietic stem or stromal cell function have been described, but the mechanisms mediating chemotherapy-induced hematopoietic dysfunction remain unclear. Administration of multiple cycles of cisplatin chemotherapy causes significant sensory neuropathy. Here, we demonstrate that chemotherapy-induced nerve injury in the bone marrow is a critical lesion impairing hematopoietic regeneration. We show using various pharmacological and genetic models that the selective loss of adrenergic innervation in the BM alters its regeneration following genotoxic insult. Sympathetic nerves in the marrow promote the survival of stem cell niche constituents that initiate recovery. Neuroprotection by deletion of Trp53 in sympathetic neurons or neuro-regeneration using 4-methylcatechol or glial-derived neurotrophic factor (GDNF) administration can restore hematopoietic recovery. Thus, these results shed light on the potential benefit of adrenergic nerve protection to shield hematopoietic niches from injury.

Published

2013

41. A niche in a dish: pericytes support HSC

Author

Jean-Pierre Levesque

Subjects

Pathology, medicine.medical_specialty, Fetus, business.industry, Hematopoiesis and Stem Cells, Immunology, Adipose tissue, Cell Biology, Hematology, CD146 Antigen, Hematopoietic Stem Cells, Biochemistry, Haematopoiesis, medicine.anatomical_structure, Cord blood, Medicine, CD146, Animals, Blood Vessels, Humans, Bone marrow, Stem cell, business, Diffuse Idiopathic Skeletal Hyperostosis

Abstract

In this issue of Blood , Corselli et al[1][1] purify CD146+ pericytes from human adipose or fetal bone marrow and demonstrate that these cells are capable of supporting the self-renewal and proliferation of transplantable human cord blood hematopoietic stem cells (HSCs). ![Figure][2] Human

Published

2013

42. Therapeutic Blockade of Macrophage Colony Stimulating Factor (CSF-1) Delays AML Progression in Mice In Vivo

Author

Valarie Barbier, Ingrid G. Winkler, Sal Lee Goh, Allison R Petitt, and Jean-Pierre Levesque

Subjects

Therapeutic blockade, Macrophage colony-stimulating factor, business.industry, Immunology, Cell Biology, Hematology, medicine.disease, Colony-stimulating factor, Biochemistry, Leukemia, Immune system, In vivo, hemic and lymphatic diseases, Precursor cell, Cancer research, medicine, business

Abstract

Macrophage colony-stimulating factor (M-CSF or CSF-1) plays a role in regulating innate immune responses promoting macrophage growth and differentiation. We hypothesized CSF-1 may also play a role in growth and progression of Acute Myeloid Leukaemia (AML). The aim of this study is to investigate the role of CSF-1 in survival and chemo-resistance of leukaemia stem and progenitor cells (LSPC). We further hypothesized that blocking CSF-1R signalling in LSPC may dampen leukaemia survival in vitro and delay leukaemia progression in vivo. AML was induced in mice by injecting murine Haematopoietic Stem and Progenitor Cells (HSPC) transduced with either MLL-AF9 or AML1- ETO fusion oncogenes for the development of either monomyelocytic or granulocytic leukaemia respectively. We found CSF-1R, the main receptor for CSF-1, was expressed on these acute myeloid leukaemia cells, thus it is possible that CSF-1 provide supportive microenvironment for leukemic growth. To identify whether CSF-1 in the bone marrow (BM) niche is essential for growth of malignant LSPC, we harvested normal or- leukaemic blasts from BM for in vitro studies using Long-Term Culture-Initiating-Cell (LT-CIC) assays. In these assays AML LSPC or normal HSPC cells were co-cultured with mesenchymal stromal cells (MSC) from either wildtype mice (MSC that produce CSF-1) or MSC from OP/OP mice (unable to produce functional CSF-1). We found normal (wild-type) HSPC were able to proliferate, survive and produce LT-CIC in the absence of niche-provided CSF-1, however AML blasts could not, unless rescued by addition of recombinant CSF-1 (100 ng/mL) in vitro. Together these data suggest CSF-1 signalling may be critical for AML LSPC but not normal HSPC. Next we investigated in mice whether therapeutic CSF-1 blockade could similarly dampen AML survival or progression in vivo. Cohorts of mice were injected with luciferase-expressing monomyelocytic (MLL-AF9) BM leukaemic blasts, then 7 days later administered the small molecule CSF-1 antagonist (GW2580, 160mg/kg daily for 10 days) or vehicle control. Leukaemia progression was tracked by biweekly bioluminescence and testbleeds for appearance of GFP+ leukaemia blasts in blood. We found therapeutic blockade of CSF-1 significantly reduced tumour burden in these mice by both bioluminescence and testbleed analysis. Mice were also monitored for duration of survival. As anticipated by the observed reduction in leukaemia burden, therapeutic CSF-1 blockade also significantly extended the duration of overall mouse survival (P Together these studies suggest therapeutic CSF-1 blockade may show promise as an adjunct therapy to help reduce tumour burden and improve success of AML leukaemia therapies. Disclosures Winkler: GlycoMimetics: Research Funding.

Published

2016

43. Pathological Heterotopic Ossifications in Brain or Spinal Cord Injured Patients: From Ectopic Bone to Hematopoietic Stem Cell Niche Development

Author

Adrienne Anginot, Bernadette Guerton, Jean-Pierre Levesque, Philippe Denormandie, Guillaume Genet, Jean-Jacques Lataillade, Nathalie Rochet, François Genet, Christophe Desterke, Erica Vlachos, Denis Clay, Marie-Caroline Le Bousse-Kerdilès, Frédéric Torossian, Nassim Arouche, and Laetitia Boutin

Subjects

Matrigel, Stromal cell, business.industry, Hematopoietic stem cell niche, Immunology, Mesenchymal stem cell, CD34, Hematopoietic stem cell, Cell Biology, Hematology, Biochemistry, medicine.anatomical_structure, Cancer research, Medicine, CD90, Progenitor cell, business

Abstract

Heterotopic ossification (HO) is a pathology characterized by the formation of ectopic bone in soft tissues generally in muscles surrounding joints such hip, knee, elbow or shoulder. The etiology of this pathology is not known but it is well established that the risk of HO is increased after traumatic brain or spinal cord injuries and also after fractures or burns. Patients with HOs suffer from pain and the range of motion from limbs with ectopic bone is highly reduced. Currently, the only effective treatment for HOs is surgery but recurrences are frequent underpinning that a better understanding of its pathophysiology is required to cure patients. Hematopoietic marrow-like tissue is frequently observed on histological section of HO. Therefore, we investigated whether HOs from patients with traumatic brain or spinal cord injury represent an ectopic model of hematopoietic stem cell (HSC) niche as defined by the presence of HSC-supportive stromal cells. HOs were obtained from patients after surgical resection in Garches Hospital (France) with their informed consent. HOs were cut in small pieces and hematopoietic as well as endothelial cells were extracted from the HO marrow by gentle washing. Mononuclear cells were then recovered by ficoll gradient and were either directly analyzed by flow cytometry or purified by immunomagnetic selection for in vitro and in vivo experiments. Mesenchymal stromal cells (MSCs) were obtained by plastic adherence from HO explants. We first confirmed the presence of hematopoietic cells from different lineages in HO marrow such as neutrophils, monocytes/macrophages, B and T lymphocytes as evidenced by membrane expression of CD45, CD15, CD11/CD14, CD19, CD3/CD4 and CD3/CD8 antigens. HSC presence within HO marrow was further demonstrated by: (i) in vitro clonogenic assays, (ii) presence of quiescent CD45+CD34+CD38- cells with a side-population phenotype and, (iii) in vivo human hematopoietic reconstitution assays in immunodeficient NSG mice. We also show that human HO marrow contained functional MSCs and endothelial progenitors (EPs) as demonstrated by phenotypic and functional analyses. MSC expressing the classical mesenchymal markers CD73, CD90, CD105 and capable to in vitro and in vivo differentiate into osteoblasts, adipocytes and chondrocytes could be isolated from human HOs. These MSCs were also able to support in vitro long term human hematopoiesis and in vivo murine hematopoiesis when seeded on hydroxyapatite scaffolds and implanted into nude mice. Endothelial progenitors with a characteristic CD31+CD144+CD34+CD45-CD90+ phenotype were detected in the mononuclear cell fraction from HO marrows. After sorting, these cells were able to form colonies on plastic and vascular networks when cultured in a Matrigel and to express high levels of VCAM-1 and ICAM-1 adhesion molecules after TNFα stimulation, confirming their EP functional capability. In conclusion, we show for the first time that human HOs contain a marrow tissue with quiescent HSC that can proliferate and differentiate within a suitable and functional mesenchymal and endothelial microenvironment, acknowledging that HO marrows are ectopic HSC niches. We have recently demonstrated the involvement of macrophages in the development of neurogenic HOs in spinalized mice1. Taking into account the role of immune cells and the neurogenic origin of human HOs, our results bring new evidences for the role of interactions between bone and neuro-immune systems in the initiation and development of adult hematopoiesis. Mechanisms underlying these processes are currently studied in our laboratory. 1 Genet F et al., J Pathol. 2015 Jun;236(2):229-40 Disclosures No relevant conflicts of interest to declare.

Published

2016

44. Suppression of Medullar Erythropoiesis in Response to Bacterial Lipopolysaccharides (LPS) Involves Two Distinct TLR4-Dependent Mechanisms with Contrasted Requirements for G-CSF Receptors

Author

Ingrid G. Winkler, Marion Brunck, Bianca Nowlan, Rebecca Jacobsen, Thomas Keech, Crystal McGirr, Kavita Bisht, and Jean-Pierre Levesque

Subjects

medicine.medical_specialty, Immunology, Spleen, Cell Biology, Hematology, Biology, Biochemistry, chemistry.chemical_compound, Endocrinology, medicine.anatomical_structure, Integrin alpha M, chemistry, Erythroblast, Hepcidin, Internal medicine, medicine, TLR4, biology.protein, Erythropoiesis, Receptor, Evans Blue

Abstract

Erythropoiesis is a highly controlled process partly regulated in erythroblastic islands by the central erythroblastic island macrophage (EI MΦ) which provides iron, growth factors and mediates enucleation of the maturing erythroblasts. As macrophages are key effectors of inflammation, we investigated the effect of bacterial LPS in vivo on erythropoiesis and EI MΦ defined as CD11b+ F4/80+ VCAM1+ CD169+Ly6G+ in mice. C57BL/6 mice were injected i.p. with 2.5 mg/kg/day LPS from E. coli for 2 days and the effect on medullar erythropoiesis examined at various time-points after this. LPS administration caused a marked whitening of the bone marrow (BM) with decreased numbers of basophilic (9-fold), polychromatic (3.7-fold), orthochromatic erythroblasts (2.2-fold) and reticulocytes (2.5-fold) 48hrs after LPS challenge. Those remained significantly reduced up to 6 days post-LPS. Likewise, EI MΦ were suppressed in the BM 24-48hrs after LPS challenge and remained significantly reduced 6 days post-LPS. This loss of medullar erythropoiesis was compensated by increased number of EI MΦ (13.6-fold), pro-erythroblasts (1.5-fold), polychromatic (1.9-fold), orthochromatic (3.2-fold) and reticulocytes (2.3-fold) in the spleen. As this phenotype resembled suppression of medullar erythropoiesis following G-CSF treatment, we examined whether the mechanism could be indirect via endogenous G-CSF release. LPS induced a transient 80-fold increase in G-CSF concentration in the blood from 123pg/mL (n=6) to 10ng/ml (n=6) 2 days post-LPS. LPS was administered to TLR4 KO and G-CSF receptor (GCSFR) KO mice. These LPS-mediated responses were abrogated in TLR4 KO mice demonstrating that erythropoiesis suppression in response to LPS is fully TLR4-dependant. However responses in GCSFR KO mice were more contrasted. EI MΦ numbers did not change in GCSFR KO mice in response to LPS demonstrating that suppression of EI MΦ in response to LPS is an indirect effect of endogenous G-CSF release. In contrast, medullar erythropoiesis was still suppressed in GCSFR KO mice with significantly reduced numbers of basophilic, polychromatic and orthochromatic erythroblasts demonstrating that medullar erythroblast suppression 1) persists despite the presence of EI MΦ, and 2) is not G-CSF-dependent. Unexpectedly, the BM from GCSFR KO mice treated with LPS was not whitened with high numbers of reticulocytes/erythrocytes. To further understand how BM erythrocytes could be increased whilst erythropoiesis is suppressed in LPS-treated GCSFR KO mice, we measured vascular leakage by injecting Evans Blue i.v. Blood plasma volume in the BM of LPS-treated GCSFR KO mice was 2.9-fold higher compared to LPS-treated wild-type mice and untreated WT and KO mice (6.0±2.0 µL vs 2.1±0.9 µL blood plasma/femur, p=0.005) suggesting that GCSFR-mediated signaling is necessary to maintain the integrity of the BM vasculature in response to LPS. In conclusion LPS-mediated medullar erythropoiesis suppression involves at least two different TLR4-dependent mechanisms in regards to their requirement for GCSFR: 1) GCSFR-dependent suppression of EI MΦ, 2) GCSFR-independent and EI MΦ-independent suppression of maturing erythroblasts. We are currently investigating whether the latter mechanism involves hepcidin. Finally we also discovered that GCSFR-mediated signaling is necessary to maintain the BM vasculature integrity following LPS challenge. Disclosures Winkler: GlycoMimetics: Research Funding. Levesque:GlycoMimetics: Equity Ownership.

Published

2016

45. Vascular E-Selectin Protects Leukemia Cells from Chemotherapy By Directly Activating Pro-Survival NF-Kb Signalling - Therapeutic Blockade of E-Selectin Dampens NF-Kb Activation

Author

Julie M. Davies, Johanna Erbani, John L. Magnani, Valerie Barbier, Micheal S. Ward, Michael R. Tallack, Ingrid G. Winkler, Jessica Lowe, and Jean-Pierre Levesque

Subjects

0301 basic medicine, biology, Cell adhesion molecule, Immunology, Myeloid leukemia, Cell Biology, Hematology, medicine.disease, Biochemistry, Transplantation, 03 medical and health sciences, Haematopoiesis, Leukemia, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, E-selectin, biology.protein, medicine, Cancer research, Cytarabine, Stem cell, medicine.drug

Abstract

The vascular adhesion molecule E-selectin is a key component of the Bone Marrow (BM) Haematopoietic Stem Cell (HSC) niche prompting HSC to proliferate at the expense of self-renewal (Winkler, Nat Med 2012).Only 3 - 5% of BM endothelial cells express E-selectin in steady state however E-selectin is greatly upregulated (5 - 10 fold) in BM of mice with acute myeloid leukemia (AML) raising the question; how do AML stem cells (LSC) respond to E-selectin at the vascular niche & does E-selectin signalling in AML & HSC differ? Using models of murine AML generated by retroviral transduction of MLL-AF9 or AML1-ETO oncogenes, we found leukemic blasts rapidly upregulate E-selectin-binding upon oncogenic transformation. Furthermore E-selectin adhesion promoted LSC survival to cytarabine in vitro as well as in vivo. LSC survival to chemotherapy in wildtype compared to E-selectin knockout (E-/-) mice quantified by rigorous limiting-dilution transplantation assay of 1%, 0.1%, 0.01% femur BM demonstrated that E-selectin deletion increased sensitivity of LSC to high-dose cytarabine therapy ~11-fold (900mg/kg cytarabine n=6 donors &15 recipients/gp p=0.0037). Thus E-selectin is a critical vascular niche component mediating LSC chemo resistance. Importantly these findings could be replicated by administration of a potent small molecule glycomimetic E-selectin antagonist (GMI-1271) to wt mice. Furthermore treatment with GMI-1271 (40mg/kg bidaily) for 10 days in combination with standard mouse version of 7+3 induction chemotherapy (5 days cytarabine 100mg/kg; 3 days doxorubicin 1mg/kg) was able to significantly double mouse survival over chemotherapy alone (p=0.0054; no chemotherapy median survival 25 d, AraC/Dox alone 32 d, AraC/Dox plus GMI-1271 survival 41 d; n=8 mice/gp). To understand mechanisms of this chemo-sensitisation, mice with MLL-AF9 monomyelocytic (11q23 translocation) or AML1-ETO granulocytic t(8;21) -induced AML were administered GMI-1271 or vehicle control for 5 days before sorting BM AML blasts for RNA sequencing. Analysis of differentially expressed transcripts by CuffDiff / DSeq2 revealed 170 RNAs differed following in vivo E-selectin blockade. KEGG pathway analysis indicated a pathway potentially dampened in AML blasts following GMI-1271 administration was PI3K - NF-kB signalling - raising the hypothesis that adhesion to E-selectin activates pro-survival NF-kB signalling in AML cells leading to enhanced chemoresistance. Using two in vitro assays, we confirmed E-selectin to be unique among vascular adhesion molecules tested in being able to directly activate NF-kB. Activation of NF-kB was only observed upon E-selectin mediated adhesion & was not observed following adhesion to P-selectin, PECAM-1 or VCAM-1 using either myeloid NF-kB GFP reporter cell lines or by induction of p65 NF-kB (Ser 536). Importantly E-selectin mediated NF-kB activation was completely inhibited when E-selectin antagonist GMI-1271 added. Assays repeated in presence of a specific NF-kB activation antagonist (BMS-345541 10uM 24hrs) demonstrated that NF-kB blockade alone reversed E-selectin-mediated chemoresistance in vitro. Upstream blockade of E-selectin by GMI-1271 not only inhibits NF-kB activation but also mobilizes LSC out of the protective BM niche & prevents re-entry thereby breaking the chemo resistance observed with these cells. A Phase I/II Clinical trial to study efficacy of GMI-1271 in combination with chemotherapy in AML patients (NCT02306291) is currently in progress Disclosures Winkler: GlycoMimetics: Research Funding. Magnani:GlycoMimetics: Employment, Equity Ownership, Membership on an entity's Board of Directors or advisory committees. Levesque:GlycoMimetics: Equity Ownership.

Published

2016

46. Hematopoietic stem cell mobilization and erythropoiesis suppression in response to lipopolysaccharides involve two distinct TLR4-depedent mechanisms with different requirement for G-CSF receptors

Author

Marion E. G. Brunck, Kavita Bisht, Crystal McGirr, Rebecca Jacobsen, Thomas Keech, Ingrid G. Winkler, Bianca Nowlan, Jean-Pierre Levesque, and Valerie Barbier

Subjects

0301 basic medicine, Cancer Research, CSF Receptors, Cell Biology, Hematology, Biology, Cell biology, 03 medical and health sciences, 030104 developmental biology, Immunology, Genetics, TLR4, Erythropoiesis, Molecular Biology, Hematopoietic Stem Cell Mobilization

Published

2016

47. Therapeutic blockade of macrophage colony stimulating factor (CSF-1) delays leukaemia progression of AML in mice in vivo

Author

Allison R. Pettit, Cecile Jeanclos, Ingrid G. Winkler, Jean-Pierre Levesque, Sal Lee Goh, and Valerie Barbier

Subjects

Macrophage colony-stimulating factor, Therapeutic blockade, Cancer Research, business.industry, In vivo, Immunology, Genetics, Medicine, Cell Biology, Hematology, business, Molecular Biology

Published

2016

48. Mobilization of hematopoietic stem cells with highest self-renewal by G-CSF precedes clonogenic cell mobilization peak

Author

Eliza Wiercinska, Ingrid G. Winkler, Halvard Bonig, Bianca Nowlan, Valerie Barbier, and Jean-Pierre Levesque

Subjects

Male, 0301 basic medicine, Cancer Research, Time Factors, medicine.medical_treatment, CD34, Hematopoietic stem cell transplantation, Biology, Immunophenotyping, Andrology, Mice, 03 medical and health sciences, 0302 clinical medicine, Granulocyte Colony-Stimulating Factor, Genetics, medicine, Animals, Humans, Cell Self Renewal, Molecular Biology, Hematopoietic Stem Cell Mobilization, Cell Cycle, Graft Survival, Hematopoietic Stem Cell Transplantation, Cell Biology, Hematology, Flow Cytometry, Hematopoietic Stem Cells, Granulocyte colony-stimulating factor, Transplantation, Haematopoiesis, Phenotype, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, Female, Bone marrow, Stem cell

Abstract

Harvest of granulocyte colony-stimulating factor (G-CSF)-mobilized hematopoietic stem cells (HSCs) begins at day 5 of G-CSF administration, when most donors have achieved maximal mobilization. This is based on surrogate markers for HSC mobilization, such as CD34(+) cells and colony-forming activity in blood. However, CD34(+) cells or colony-forming units in culture (CFU-C) are heterogeneous cell populations with hugely divergent long-term repopulation potential on transplantation. HSC behavior is influenced by the vascular bed in the vicinity of which they reside. We hypothesized that G-CSF may mobilize sequentially cells proximal and more distal to bone marrow venous sinuses where HSCs enter the blood. We addressed this question with functional serial transplantation assays using blood and bone marrow after specific time points of G-CSF treatment in mice. We found that in mice, blood collected after only 48 hours of G-CSF administration was as enriched in serially reconstituting HSCs as blood collected at 5 days of G-CSF treatment. Similarly, mobilized Lin(-)CD34(+) cells were relatively enriched in more primitive Lin(-)CD34(+)CD38(-) cells at day 2 of G-CSF treatment compared with later points in half of human donors tested (n = 6). This suggests that in both humans and mice, hematopoietic progenitor and stem cells do not mobilize uniformly according to their maturation stage, with most potent HSCs mobilizing as early as day 2 of G-CSF.

Published

2016

49. Pharmacologic stabilization of HIF-1α increases hematopoietic stem cell quiescence in vivo and accelerates blood recovery after severe irradiation

Author

Valerie Barbier, Bianca Nowlan, Ingrid G. Winkler, Gail Walkinshaw, Jean-Pierre Levesque, and Catherine E. Forristal

Subjects

Male, Cell Survival, Immunology, Biology, Biochemistry, Resting Phase, Cell Cycle, Mice, In vivo, medicine, Animals, Protease Inhibitors, Transcription factor, Erythropoietin, Regulation of gene expression, Hematopoietic stem cell, Cell Biology, Hematology, Hypoxia (medical), Cell cycle, Hematopoietic Stem Cells, Hypoxia-Inducible Factor 1, alpha Subunit, Cell biology, Amino Acids, Dicarboxylic, Haematopoiesis, Radiation Injuries, Experimental, medicine.anatomical_structure, Gene Expression Regulation, Gamma Rays, Proteolysis, medicine.symptom, Stem cell

Abstract

Quiescent hematopoietic stem cells (HSCs) preferentially reside in poorly perfused niches that may be relatively hypoxic. Most of the cellular effects of hypoxia are mediated by O2-labile hypoxia-inducible transcription factors (HIFs). To investigate the effects of hypoxia on HSCs, we blocked O2-dependent HIF-1α degradation in vivo in mice by injecting 2 structurally unrelated prolyl hydroxylase domain (PHD) enzyme inhibitors: dimethyloxalyl glycine and FG-4497. Injection of either of these 2 PHD inhibitors stabilized HIF-1α protein expression in the BM. In vivo stabilization of HIF-1a with these PHD inhibitors increased the proportion of phenotypic HSCs and immature hematopoietic progenitor cells in phase G0 of the cell cycle and decreased their proliferation as measured by 5-bromo-2'-deoxyuridine incorporation. This effect was independent of erythropoietin, the expression of which was increased in response to PHD inhibitors. Finally, pretreatment of mice with a HIF-1α stabilizer before severe, sublethal 9.0-Gy irradiation improved blood recovery and enhanced 89-fold HSC survival in the BM of irradiated mice as measured in long-term competitive repopulation assays. The results of the present study demonstrate that the levels of HIF-1α protein can be manipulated pharmacologically in vivo to increase HSC quiescence and recovery from irradiation.HIF-1α protein stabilization increases HSC quiescence in vivo. HIF-1α protein stabilization increases HSC resistance to irradiation and accelerates recovery.

Published

2012

50. N(o)-cadherin role for HSCs

Author

Jean-Pierre Levesque

Subjects

Cell adhesion molecule, Cadherin, Hematopoiesis and Stem Cells, Immunology, Hematopoietic stem cell, hemic and immune systems, Cell Biology, Hematology, Adhesion, Biology, Biochemistry, Cell biology, Haematopoiesis, medicine.anatomical_structure, medicine, Ex vivo expansion, Gene

Abstract

Hematopoietic stem cell (HSC) regulation is highly dependent on interactions with the marrow microenvironment. Controversy exists on N-cadherin's role in support of HSCs. Specifically, it is unknown whether microenvironmental N-cadherin is required for normal marrow microarchitecture and for hematopoiesis. To determine whether osteoblastic N-cadherin is required for HSC regulation, we used a genetic murine model in which deletion of Cdh2, the gene encoding N-cadherin, has been targeted to cells of the osteoblastic lineage. Targeted deletion of N-cadherin resulted in an age-dependent bone phenotype, ultimately characterized by decreased mineralized bone, but no difference in steady-state HSC numbers or function at any time tested, and normal recovery from myeloablative injury. Intermittent parathyroid hormone (PTH) treatment is well established as anabolic to bone and to increase marrow HSCs through microenvironmental interactions. Lack of osteoblastic N-cadherin did not block the bone anabolic or the HSC effects of PTH treatment. This report demonstrates that osteoblastic N-cadherin is not required for regulation of steady-state hematopoiesis, HSC response to myeloablation, or for rapid expansion of HSCs through intermittent treatment with PTH.

Published

2012